BLINCYTO®
(blinatumomab) for Injection
WARNING
CYTOKINE RELEASE SYNDROME and NEUROLOGICAL TOXICITIES
·
Cytokine
Release Syndrome (CRS), which may be life-threatening or fatal, occurred in
patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended
[see DOSAGE AND
ADMINISTRATION, WARNINGS AND PRECAUTIONS].
·
Neurological
toxicities, which may be severe, life-threatening, or fatal, occurred in
patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended
[see DOSAGE AND
ADMINISTRATION, WARNINGS AND PRECAUTIONS].
DESCRIPTION
BLINCYTO
(blinatumomab) is a bispecific CD19-directed CD3 T-cell engager that binds to
CD19 (expressed on cells of B-lineage origin) and CD3 (expressed on T cells).
BLINCYTO is produced in Chinese hamster ovary cells. It consists of 504 amino acids and has a molecular weight of
approximately 54 kilodaltons.
Each
BLINCYTO package contains 1 vial BLINCYTO and 1 vial IV Solution Stabilizer.
BLINCYTO
is supplied in a single-dose vial as a sterile, preservative-free, white to
off-white lyophilized powder for intravenous administration. Each single-dose
vial of BLINCYTO contains 35 mcg blinatumomab, citric acid monohydrate (3.35
mg), lysine hydrochloride (23.23 mg),
polysorbate 80 (0.64 mg), trehalose dihydrate (95.5 mg), and sodium hydroxide
to adjust pH to 7.0. After reconstitution with 3 mL of preservative-free
Sterile Water for Injection, USP, the resulting concentration is 12.5 mcg/mL
blinatumomab.
IV
Solution Stabilizer is supplied in a single-dose vial as a sterile,
preservative-free, colorless to slightly yellow, clear solution. Each
single-dose vial of IV Solution Stabilizer contains citric acid monohydrate
(52.5 mg), lysine hydrochloride (2283.8 mg), polysorbate 80 (10 mg), sodium
hydroxide to adjust pH to 7.0, and water for injection.
INDICATIONSMRD-positive B-cell Precursor ALL
BLINCYTO
is indicated for the treatment of B-cell precursor acute lymphoblastic leukemia (ALL) in
first or second complete remission with minimal residual disease (MRD) greater than or equal to 0.1% in adults
and children.
This
indication is approved under accelerated approval based on MRD response rate
and hematological relapse-free survival. Continued approval for this indication
may be contingent upon verification and description of clinical benefit in the
confirmatory trials.
Relapsed Or Refractory B-cell Precursor ALL
BLINCYTO
is indicated for the treatment of relapsed or refractory B-cell precursor acute
lymphoblastic leukemia (ALL) in adults and children.
DOSAGE AND
ADMINISTRATIONTreatment Of MRD-Positive B-cell Precursor ALL
·
A treatment course consists of 1 cycle of BLINCYTO for induction
followed by up to 3 additional cycles for consolidation.
·
A single cycle of treatment of BLINCYTO induction or
consolidation consists of 28 days of continuous intravenous infusion followed
by a 14-day treatment-free interval (total 42 days).
·
See Table 1 for the recommended dose by patient weight and
schedule. Patients greater than or equal to 45 kg receive a fixed-dose. For
patients less than 45 kg, the dose is calculated using the patient's body
surface area (BSA).
Table 1: Recommended BLINCYTO Dosage and
Schedule for the Treatment of MRD-positive B-cell Precursor ALL
|
Cycle
|
Patient Weight Greater Than or
Equal to 45 kg (Fixed-dose)
|
Patient Weight Less Than 45 kg
(BSA-based dose)
|
|
Induction Cycle 1
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Consolidation Cycles 2-4
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
·
Hospitalization is recommended for the first 3 days of the first
cycle and the first 2 days of the second cycle. For all subsequent cycle starts
and re-initiations (e.g., if treatment is interrupted for 4 or more hours),
supervision by a healthcare professional or hospitalization is recommended.
·
Premedicate with prednisone or equivalent for MRD-positive
B-cell Precursor ALL
o For adult
patients, premedicate with prednisone 100 mg intravenously or equivalent
(e.g., dexamethasone 16 mg) 1 hour prior to the
first dose of BLINCYTO in each cycle.
o For pediatric
patients, premedicate with 5 mg/m² of dexamethasone, to a maximum dose of 20 mg
prior to the first dose of BLINCYTO in the first cycle and when restarting an
infusion after an interruption of 4 or more hours in the first cycle.
·
For administration of BLINCYTO:
o See Section
2.5 for infusion over 24 hours or 48 hours.
o See Section
2.6 for infusion over 7 days using Bacteriostatic 0.9% Sodium Chloride
Injection, USP (containing 0.9% benzyl alcohol). This option is available for
patients weighing greater than or equal to 22 kg. It is not recommended for use
in patients weighing less than 22 kg.
Treatment Of Relapsed Or Refractory B-cell Precursor ALL
·
A treatment course consists of up to 2 cycles of BLINCYTO for
induction followed by 3 additional cycles for consolidation and up to 4 additional
cycles of continued therapy.
·
A single cycle of treatment of BLINCYTO induction or
consolidation consists of 28 days of continuous intravenous infusion followed
by a 14-day treatment-free interval (total 42 days).
·
A single cycle of treatment of BLINCYTO continued therapy
consists of 28 days of continuous intravenous infusion followed by a 56-day
treatment-free interval (total 84 days).
·
See Table 2 for the recommended dose by patient weight and
schedule. Patients greater than or equal to 45 kg receive a fixed-dose and for
patients less than 45 kg, the dose is calculated using the patient's body
surface area (BSA).
Table 2: Recommended BLINCYTO Dosage and
Schedule for the Treatment of Relapsed or Refractory B-cell Precursor ALL
|
Cycle
|
Patient Weight Greater Than or
Equal to 45 kg (Fixed-dose)
|
Patient Weight Less Than 45 kg
(BSA-based dose)
|
|
Induction Cycle 1
|
|
Days 1-7
|
9 mcg/day
|
5 mcg/m²/day (not to exceed 9 mcg/day)
|
|
Days 8-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Induction Cycle 2
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Consolidation Cycles 3-5
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Continued Therapy Cycles 6-9
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-84
|
56-day treatment-free interval
|
56-day treatment-free interval
|
·
Hospitalization is recommended for the first 9 days of the first
cycle and the first 2 days of the second cycle. For all subsequent cycle starts
and re-initiation (e.g., if treatment is interrupted for 4 or more hours),
supervision by a healthcare professional or hospitalization is recommended.
·
Premedicate with dexamethasone.
o For adult
patients, premedicate with 20 mg dexamethasone 1 hour prior to the first dose
of BLINCYTO of each cycle, prior to a step dose (such as Cycle 1 Day 8), and
when restarting an infusion after an interruption of 4 or more hours.
o For pediatric
patients, premedicate with 5 mg/m² of dexamethasone, to a maximum dose of 20 mg
prior to the first dose of BLINCYTO in the first cycle, prior to a step dose
(such as Cycle 1 Day 8), and when restarting an infusion after an interruption
of 4 or more hours in the first cycle.
·
For administration of BLINCYTO:
o See Section
2.5 for infusion over 24 hours or 48 hours.
o See Section
2.6 for infusion over 7 days using Bacteriostatic 0.9% Sodium Chloride
Injection, USP (containing 0.9% benzyl alcohol). This option is available for
patients weighing greater than or equal to 22 kg. It is not recommended for use
in patients weighing less than 22 kg.
Dosage Adjustments
If
the interruption after an adverse event is no longer than 7 days, continue the
same cycle to a total of 28 days of infusion inclusive of days before and after
the interruption in that cycle. If an interruption due to an adverse event is
longer than 7 days, start a new cycle.
Table 3: Dose Modifications for Toxicity
|
Toxicity
|
Grade*
|
Patients Greater Than or Equal
to 45 kg
|
Patients Less Than 45 kg
|
|
Cytokine Release Syndrome (CRS)
|
Grade 3
|
Withhold BLINCYTO until resolved, then
restart BLINCYTO at 9 mcg/day. Escalate to 28 mcg/day after 7 days if the
toxicity does not recur.
|
Withhold BLINCYTO until resolved, then
restart BLINCYTO at 5 mcg/m²/day. Escalate to 15 mcg/m²/day after 7 days if
the toxicity does not recur.
|
|
|
Grade 4
|
Discontinue BLINCYTO permanently.
|
|
Neurological Toxicity
|
Seizure
|
Discontinue BLINCYTO permanently if more
than one seizure occurs.
|
|
|
Grade 3
|
Withhold BLINCYTO until no more than Grade
1 (mild) and for at least 3 days, then restart BLINCYTO at 9 mcg/day.
Escalate to 28 mcg/day after 7 days if the toxicity does not recur. If the
toxicity occurred at 9 mcg/day, or if the toxicity takes more than 7 days to
resolve, discontinue BLINCYTO permanently.
|
Withhold BLINCYTO until no more than Grade
1 (mild) and for at least 3 days, then restart BLINCYTO at 5 mcg/m²/day.
Escalate to 15 mcg/m²/day after 7 days if the toxicity does not recur. If the
toxicity occurred at 5 mcg/m²/day, or if the toxicity takes more than 7 days
to resolve, discontinue BLINCYTO permanently.
|
|
Toxicity
|
Grade*
|
Patients Greater Than or Equal to 45 kg
|
Patients Less Than 45 kg
|
|
|
Grade 4
|
Discontinue BLINCYTO permanently.
|
|
Other Clinically Relevant Adverse
Reactions
|
Grade 3
|
Withhold BLINCYTO until no more than Grade
1 (mild), then restart BLINCYTO at 9 mcg/day. Escalate to 28 mcg/day after 7
days if the toxicity does not recur. If the toxicity takes more than 14 days
to resolve, discontinue BLINCYTO permanently.
|
Withhold BLINCYTO until no more than Grade
1 (mild), then restart BLINCYTO at 5 mcg/m²/day. Escalate to 15 mcg/m²/day
after 7 days if the toxicity does not recur. If the toxicity takes more than
14 days to resolve, discontinue BLINCYTO permanently.
|
|
|
Grade 4
|
Consider discontinuing BLINCYTO
permanently.
|
|
* Based on the Common Terminology Criteria
for Adverse Events (CTCAE). Grade 3 is severe, and Grade 4 is
life-threatening.
|
Preparation
It
is very important that the instructions for preparation (including admixing)
and administration provided in this section are strictly followed to minimize
medication errors (including underdose and overdose) [see WARNINGS
AND PRECAUTIONS].
BLINCYTO
can be infused over 24 hours (preservative-free) or 48 hours
(preservative-free), or 7 days (with preservative). The choice between these
options for the infusion duration should be made by the treating physician
considering the frequency of the infusion bag changes and the weight of the
patient. The 7-day infusion is not recommended for patients weighing less than
22 kg.
For
preparation, reconstitution, and administration of BLINCYTO:
·
See Section 2.5 for infusion over 24 hours or 48 hours.
·
See Section 2.6 for infusion over 7 days using Bacteriostatic
0.9% Sodium Chloride Injection, USP (containing 0.9% benzyl alcohol). This
option is available for patients weighing greater than or equal to 22 kg. It is
not recommended for patients weighing less than 22 kg.
Call
1-800-77-AMGEN (1-800-772-6436) if you have questions about the reconstitution
and preparation of BLINCYTO.
Aseptic Preparation
Strictly
observe aseptic technique when preparing the
solution for infusion since BLINCYTO vials do not contain antimicrobial preservatives. To prevent
accidental contamination, prepare BLINCYTO according to aseptic standards,
including but not limited to:
·
Prepare BLINCYTO in a USP <797> compliant facility.
·
Prepare BLINCYTO in an ISO Class 5 laminar flow hood or better.
·
Ensure that the admixing area has appropriate environmental
specifications, confirmed by periodic monitoring.
·
Ensure that personnel are appropriately trained in aseptic
manipulations and admixing of oncology drugs.
·
Ensure that personnel wear appropriate protective clothing and
gloves.
·
Ensure that gloves and surfaces are disinfected.
Package Content
1
package BLINCYTO includes 1 vial of BLINCYTO and 1 vial of IV Solution
Stabilizer.
·
Do not use IV Solution Stabilizer for reconstitution of
BLINCYTO. IV Solution Stabilizer is provided with the BLINCYTO package and
is used to coat the IV bag prior to addition of reconstituted BLINCYTO to
prevent adhesion of BLINCYTO to IV bags and IV
tubing.
·
More than 1 package of BLINCYTO may be needed to prepare some of
the prescribed doses.
Incompatibility Information
BLINCYTO
is incompatible with di-ethylhexylphthalate (DEHP) due to the possibility of particle
formation, leading to a cloudy solution.
·
Use polyolefin, PVC DEHP-free, or ethyl vinyl acetate
(EVA) infusion bags/pump cassettes.
·
Use polyolefin, PVC DEHP-free, or EVA IV tubing sets.
24-Hour Or 48-Hour Infusion Of BLINCYTOPreparation Of BLINCYTO Infusion Bag For 24- Or 48-Hour
Infusion
Verify
the prescribed dose and infusion duration for each BLINCYTO infusion bag. To
minimize errors, use the specific volumes described in Tables 4 to 6 to
prepare the BLINCYTO infusion bag.
·
Table 4 for patients weighing greater than or equal to 45 kg
·
Tables 5 and 6 for patients weighing less than 45 kg
Aseptically
add 270 mL 0.9% Sodium Chloride Injection, USP to the IV bag.Aseptically
transfer 5.5 mL IV Solution Stabilizer to the IV bag containing 0.9%
Sodium Chloride Injection, USP. Gently mix the contents of the bag to
avoid foaming. Discard the vial containing the unused IV Solution
Stabilizer.Aseptically
transfer reconstituted BLINCYTO [see Reconstitution of BLINCYTO]
into the IV bag containing 0.9% Sodium Chloride Injection, USP and IV
Solution Stabilizer. Gently mix the contents of the bag to avoid foaming.
o Refer to
Tables 4 to 6 for the specific volume of reconstituted BLINCYTO.
Under
aseptic conditions, attach the IV tubing to the IV bag with the sterile
0.2 micron in-line filter.
o Ensure that
the IV tubing is compatible with the infusion pump.
Remove
air from the IV bag. This is particularly important for use with an
ambulatory infusion pump. Prime the IV tubing only with the prepared
solution for infusion. Do not prime with 0.9% Sodium Chloride Injection,
USP.Store
at 2°C to 8°C if not used immediately [see DOSAGE AND
ADMINISTRATION].
Table 4: For Patients Weighing Greater Than
or Equal to 45 kg: Volumes to Add to IV Bag
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
Reconstituted BLINCYTO
|
|
9 mcg/day
|
24 hours
|
10 mL/hour
|
0.83 mL
|
|
48 hours
|
5 mL/hour
|
1.7 mL
|
|
28 mcg/day
|
24 hours
|
10 mL/hour
|
2.6 mL
|
|
48 hours
|
5 mL/hour
|
5.2 mL*
|
|
* 2 packages of BLINCYTO are needed for
preparation of 28 mcg/day dose infused over 48 hours at a rate of 5 mL/hour.
|
Table 5: For Patients Weighing Less Than 45
kg: Volumes to Add to IV Bag for 5 mcg/m²/day Dose
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
BSA (m²)
|
Reconstituted BLINCYTO
|
|
5 mcg/m²/day
|
24 hours
|
10 mL/hour
|
1.5 - 1.59
|
0.7 mL
|
|
1.4 - 1.49
|
0.66 mL
|
|
1.3 - 1.39
|
0.61 mL
|
|
1.2 - 1.29
|
0.56 mL
|
|
1.1 - 1.19
|
0.52 mL
|
|
1 - 1.09
|
0.47 mL
|
|
0.9 - 0.99
|
0.43 mL
|
|
0.8 - 0.89
|
0.38 mL
|
|
0.7 - 0.79
|
0.33 mL
|
|
0.6 - 0.69
|
0.29 mL
|
|
0.5 - 0.59
|
0.24 mL
|
|
0.4 - 0.49
|
0.2 mL
|
|
5 mcg/m²/day
|
48 hours
|
5 mL/hour
|
1.5 - 1.59
|
1.4 mL
|
|
1.4 - 1.49
|
1.3 mL
|
|
1.3 - 1.39
|
1.2 mL
|
|
1.2 - 1.29
|
1.1 mL
|
|
1.1 - 1.19
|
1 mL
|
|
1 - 1.09
|
0.94 mL
|
|
0.9 - 0.99
|
0.85 mL
|
|
0.8 - 0.89
|
0.76 mL
|
|
0.7 - 0.79
|
0.67 mL
|
|
0.6 - 0.69
|
0.57 mL
|
|
0.5 - 0.59
|
0.48 mL
|
|
0.4 - 0.49
|
0.39 mL
|
Table 6: For Patients Weighing Less Than 45
kg: Volumes to Add to IV Bag for 15 mcg/m²/day Dose
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
BSA (m²)
|
Reconstituted BLINCYTO
|
|
15 mcg/m²/day
|
24 hours
|
10 mL/hour
|
1.5 - 1.59
|
2.1 mL
|
|
1.4 - 1.49
|
2 mL
|
|
1.3 - 1.39
|
1.8 mL
|
|
1.2 - 1.29
|
1.7 mL
|
|
1.1 - 1.19
|
1.6 mL
|
|
1 - 1.09
|
1.4 mL
|
|
0.9 - 0.99
|
1.3 mL
|
|
0.8 - 0.89
|
1.1 mL
|
|
0.7 - 0.79
|
1 mL
|
|
0.6 - 0.69
|
0.86 mL
|
|
0.5 - 0.59
|
0.72 mL
|
|
0.4 - 0.49
|
0.59 mL
|
|
15 mcg/m²/day
|
48 hours
|
5 mL/hour
|
1.5 - 1.59
|
4.2 mL*
|
|
1.4 - 1.49
|
3.9 mL*
|
|
1.3 - 1.39
|
3.7 mL*
|
|
1.2 - 1.29
|
3.4 mL*
|
|
1.1 - 1.19
|
3.1 mL*
|
|
1 - 1.09
|
2.8 mL
|
|
0.9 - 0.99
|
2.6 mL
|
|
0.8 - 0.89
|
2.3 mL
|
|
0.7 - 0.79
|
2 mL
|
|
0.6 - 0.69
|
1.7 mL
|
|
0.5 - 0.59
|
1.4 mL
|
|
0.4 - 0.49
|
1.2 mL
|
|
* 2 packages of BLINCYTO are needed for
preparation of 15 mcg/m²/day dose infused over 48 hours at a rate of 5
mL/hour for patients with a BSA greater than 1.09 m².
|
Reconstitution Of BLINCYTOAdd
3 mL of preservative-free Sterile Water for Injection, USP by directing
the water along the walls of the BLINCYTO vial and not directly on the
lyophilized powder (resulting in a final BLINCYTO concentration of 12.5
mcg/mL).
o Do not
reconstitute BLINCYTO with IV Solution Stabilizer.
Gently
swirl contents to avoid excess foaming. Do not shake.Visually
inspect the reconstituted solution for particulate matter and
discoloration during reconstitution and prior to infusion. The resulting
solution should be clear to slightly opalescent, colorless to slightly
yellow. Do not use if solution is cloudy or has precipitated.Administration
·
Administer BLINCYTO as a continuous intravenous infusion at a
constant flow rate using an infusion pump. The pump should be programmable,
lockable, non-elastomeric, and have an alarm.
·
Prepared BLINCYTO infusion bags [see DOSAGE AND
ADMINISTRATION] should be infused over 24 hours or 48 hours.
·
The starting volume (270 mL) is more than the volume
administered to the patient (240 mL) to account for the priming of the IV
tubing and to ensure that the patient will receive the full dose of BLINCYTO.
· Infuse BLINCYTO solution according to the
instructions on the pharmacy label on the prepared bag at one of the following
constant infusion rates:
o Infusion rate
of 10 mL/hour for a duration of 24 hours, OR
o Infusion rate
of 5 mL/hour for a duration of 48 hours
·
The BLINCYTO solution must be administered using IV tubing that
contains a sterile, non-pyrogenic, low protein-binding, 0.2 micron in-line
filter.
·
Important Note: Do not flush the BLINCYTO infusion line or
intravenous catheter, especially when changing infusion bags.Flushingwhen changing bags or at completion of infusion can result in excess dosage and
complications thereof. When administering via a multi-lumen venous catheter,
BLINCYTO should be infused through a dedicated lumen.
·
At the end of the infusion, any unused BLINCYTO solution in the
IV bag and IV tubing should be disposed of in accordance with local requirements.
7-Day Infusion Of BLINCYTO Using Bacteriostatic Saline
This
option is not recommended for use in patients weighing less than 22 kg
[see WARNINGS AND PRECAUTIONS and Use
In Specific Populations].
Preparation Of BLINCYTO Infusion Bag For 7-Day Infusion
Verify
the prescribed dose and infusion duration for each BLINCYTO infusion bag. To
minimize errors, use the specific volumes described in Table 7 to prepare the
BLINCYTO infusion bag.
Aseptically
add 90 mL Bacteriostatic 0.9% Sodium Chloride Injection, USP to the empty
IV bag.Aseptically
transfer 2.2 mL IV Solution Stabilizer to the IV bag containing the saline
solution. Gently mix the contents of the bag to avoid foaming.
Discard the vial containing the unused IV Solution Stabilizer.Aseptically
transfer reconstituted BLINCYTO [see Reconstitution of BLINCYTO]
into the IV bag containing the
saline solution and IV Solution
Stabilizer. Gently mix the contents of the bag to avoid foaming.
o Refer to
Table 7 for the specific volume of reconstituted BLINCYTO.
Aseptically
add 0.9% Sodium Chloride Injection, USP to the IV bag to a final volume of
110 mL resulting in 0.74% benzyl alcohol. Gently mix the contents of
the bag to avoid foaming.
o Refer to
Table 7 for the specific volume of 0.9% Sodium Chloride Injection, USP.
Under
aseptic conditions, attach the IV tubing to the IV bag. An in-line filter
is not required for a 7-day bag.
o Ensure that
the IV tubing is compatible with the infusion pump.
Remove
air from the IV bag. This is particularly important for use with an
ambulatory infusion pump. Prime the IV tubing only with the prepared
solution for infusion. Do not prime with 0.9% Sodium Chloride Injection,
USP.Store
at 2°C to 8°C if not used immediately [see Storage Requirements].
Table 7: For 7-Day Infusion: Volumes to Add
to IV Bag for 28 mcg/day and 15 mcg/m²/day; Not Recommended for Patients Less
Than 22 kg
|
Bacteriostatic 0.9% Sodium Chloride
Injection, USP (starting volume)
|
90 mL
|
|
IV Solution Stabilizer
|
2.2 mL
|
|
Reconstituted BLINCYTO
|
Specific volume listed below in table
|
|
Quantity Sufficient (qs) with 0.9% Sodium
Chloride Injection, USP to a Final Volume of 110 mL
|
|
Infusion Duration
|
7 days
|
|
Infusion Rate
|
0.6 mL/hour
|
|
Patient Weight
|
Dose
|
BSA (m²)
|
Number of BLINCYTO Packages
|
Reconstituted BLINCYTO
|
0.9% Sodium Chloride
Injection, USP to qs to a Final Volume of 110 mL
|
|
Greater than or equal to 45 kg
(fixed-dose)
|
28 mcg/day
|
|
6
|
16.8 mL
|
1 mL
|
|
22-45 kg (BSA-based dose)
|
15 mcg/m²/day
|
1.5 - 1.59
|
5
|
14 mL
|
3.8 mL
|
|
1.4 - 1.49
|
5
|
13.1 mL
|
4.7 mL
|
|
1.30 - 1.39
|
5
|
12.2 mL
|
5.6 mL
|
|
1.20 - 1.29
|
5
|
11.3 mL
|
6.5 mL
|
|
1.10 - 1.19
|
4
|
10.4 mL
|
7.4 mL
|
|
1 - 1.09
|
4
|
9.5 mL
|
8.3 mL
|
|
0.9 - 0.99
|
4
|
8.6 mL
|
9.2 mL
|
Reconstitution Of BLINCYTOAdd
3 mL of preservative-free Sterile Water for Injection, USP by directing
the water along the walls of the BLINCYTO vial and not directly on the
lyophilized powder (resulting in a final BLINCYTO concentration of 12.5
mcg/mL).
o Do not
reconstitute BLINCYTO with IV Solution Stabilizer.
Gently
swirl contents to avoid excess foaming. Do not shake.Visually
inspect the reconstituted solution for particulate matter and
discoloration during reconstitution and prior to infusion. The resulting
solution should be clear to slightly opalescent, colorless to slightly
yellow. Do not use if solution is cloudy or has precipitated.Administration
·
Administer BLINCYTO as a continuous intravenous infusion at a
constant flow rate using an infusion pump. The pump should be programmable,
lockable, non-elastomeric, and have an alarm.
·
Prepared BLINCYTO infusion bags [see Preparation of
BLINCYTO Infusion Bag for 7-Day Infusion] should be infused over 7 days.
·
The final volume of infusion solution (110 mL) will be more than
the volume administered to the patient (100 mL) to account for the priming of
the IV tubing and to ensure that the patient will receive the full dose of
BLINCYTO.
·
Infuse BLINCYTO solution according to the instructions on the
pharmacy label on the prepared bag at an infusion rate of 0.6 mL/hour for a
duration of 7 days.
·
Important Note: Do not flush the BLINCYTO infusion line or
intravenous catheter, especially when changing infusion bags.Flushingwhen changing bags or at completion of infusion can result in excess dosage and
complications thereof. When administering via a multi-lumen venous catheter,
BLINCYTO should be infused through a dedicated lumen.
·
At the end of the infusion, any unused BLINCYTO solution in the
IV bag and IV tubing should be disposed of in accordance with local
requirements.
Storage Requirements
The
information in Table 8 indicates the storage time for the reconstituted
BLINCYTO vial and prepared infusion bag.
Store
lyophilized BLINCYTO and IV Solution Stabilizer vials for a maximum of 8 hours
at room temperature in the original carton to protect from light [see HOW
SUPPLIED/Storage And Handling].
Table 8: Storage Time for Reconstituted
BLINCYTO Vial and Prepared BLINCYTO Infusion Bag
|
|
Maximum Storage Time
|
|
Room Temperature 23°C to 27°C
(73°F to 81°F)
|
Refrigerated 2°C to 8°C (36°F
to 46°F)
|
|
Reconstituted BLINCYTO Vial
|
4 hours
|
24 hours
|
|
Prepared BLINCYTO Infusion Bag
(Preservative-Free)
|
48 hours*
|
8 days
|
|
Prepared BLINCYTO Infusion Bag (with
Preservative)
|
7 days*
|
14 days
|
|
* Storage time includes infusion time. If
the prepared BLINCYTO infusion bag is not administered within the time frames
and temperatures indicated, it must be discarded; it should not be
refrigerated again.
|
HOW SUPPLIEDDosage Forms And Strengths
For
injection: 35 mcg of lyophilized powder in a single-dose vial for
reconstitution.
Each BLINCYTO package (NDC 55513-160-01) contains:
·
One BLINCYTO 35 mcg single-dose vial containing a sterile,
preservative-free, white to off-white lyophilized powder and
·
One IV Solution Stabilizer 10 mL single-dose glass vial
containing a sterile, preservative-free, colorless to slightly yellow, clear
solution. Do not use the IV Solution Stabilizer to reconstitute BLINCYTO.
Storage And Handling
Store
BLINCYTO and IV Solution Stabilizer vials in the original package refrigerated
at 2°C to 8°C (36°F to 46°F) and protect from light until time of use. Do not
freeze.
Store
and transport the prepared IV bag containing BLINCYTO solution for infusion at
2°C to 8°C (36°F to 46°F) conditions. Ship in packaging that has been validated
to maintain temperature of the contents at 2°C to 8°C (36°F to 46°F). Do not
freeze.
Side Effects & Drug
Interactions
SIDE EFFECTS
The following adverse reactions are discussed in greater
detail in other sections of the label:
· Cytokine Release Syndrome
[see WARNINGS AND PRECAUTIONS]
· Neurological Toxicities
[see WARNINGS AND PRECAUTIONS]
· Infections [see WARNINGS
AND PRECAUTIONS]
· Tumor Lysis Syndrome [see WARNINGS
AND PRECAUTIONS]
· Neutropenia and Febrile Neutropenia [see WARNINGS
AND PRECAUTIONS]
· Effects on Ability to Drive and
Use Machines [see WARNINGS AND PRECAUTIONS]
· Elevated Liver Enzymes
[see WARNINGS AND PRECAUTIONS]
· Pancreatitis [see WARNINGS AND PRECAUTIONS]
· Leukoencephalopathy
[see WARNINGS AND PRECAUTIONS]
Clinical Trials Experience
Because clinical trials are conducted under widely varying
conditions, adverse reaction rates observed in the clinical trials of a drug
cannot be directly compared to rates in the clinical trials of another drug and
may not reflect the rates observed in practice.
MRD-Positive B-cell Precursor
ALL
The safety of BLINCYTO in patients with MRD-positive B-cell
precursor ALL was evaluated in two single-arm clinical studies in which 137
patients were treated with BLINCYTO. The median age of the study population was 45 years (range: 18
to 77 years).
The most common adverse reactions (≥ 20%) were pyrexia,
infusion related reactions, headache, infections (pathogen unspecified), tremor, and chills. Serious adverse reactions
were reported in 61% of patients. The most common serious adverse reactions (≥
2%) included pyrexia, tremor, encephalopathy, aphasia, lymphopenia, neutropenia, overdose,
device related infection, seizure, and staphylococcal infection. Adverse reactions of
Grade 3 or higher were reported in 64% of patients. Discontinuation of therapy
due to adverse reactions occurred in 17% of patients; neurologic events were
the most frequently reported reasons for discontinuation. There were 2 fatal
adverse events that occurred within 30 days of the end of BLINCYTO treatment (atypical pneumonia and subdural hemorrhage).
Table 9 summarizes the adverse reactions occurring at a ≥
10% incidence for any grade or ≥ 5% incidence for Grade 3 or higher.
Table 9: Adverse
Reactions Occurring at ≥ 10% Incidence for Any Grade or ≥ 5% Incidence for
Grade 3 or Higher in BLINCYTO-Treated Patients with MRD-Positive B-cell
Precursor ALL (N=137)
|
Adverse Reaction
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
|
Blood and lymphatic system disorders
|
|
Neutropenia1
|
21 (15)
|
21 (15)
|
|
Leukopenia2
|
19 (14)
|
13 (9)
|
|
Thrombocytopenia3
|
14 (10)
|
8 (6)
|
|
Cardiac disorders
|
|
Arrhythmia4
|
17 (12)
|
3 (2)
|
|
General disorders and administration site
conditions
|
|
Pyrexia5
|
125 (91)
|
9 (7)
|
|
Chills
|
39 (28)
|
0 (0)
|
|
Infections and infestations
|
|
Infections - pathogen unspecified
|
53 (39)
|
11 (8)
|
|
Injury, poisoning and procedural
complications
|
|
Infusion related reaction6
|
105 (77)
|
7 (5)
|
|
Investigations
|
|
Decreased immunoglobulins7
|
25 (18)
|
7 (5)
|
|
Weight increased
|
14 (10)
|
1 (<1)
|
|
Hypertransaminasemia8
|
13 (9)
|
9 (7)
|
|
Musculoskeletal and connective tissue
disorders
|
|
Back pain
|
16 (12)
|
1 (<1)
|
|
Nervous system disorders
|
|
Headache
|
54 (39)
|
5 (4)
|
|
Tremor9
|
43 (31)
|
6 (4)
|
|
Aphasia
|
16 (12)
|
1 (<1)
|
|
Dizziness
|
14 (10)
|
1 (<1)
|
|
Encephalopathy10
|
14 (10)
|
6 (4)
|
|
Psychiatric disorders
|
|
Insomnia11
|
24 (18)
|
1 (<1)
|
|
Respiratory, thoracic and mediastinal
disorders
|
|
Cough
|
18 (13)
|
0 (0)
|
|
Skin and subcutaneous tissue disorders
|
|
Rash12
|
22 (16)
|
1 (<1)
|
|
Vascular disorders
|
|
Hypotension
|
19 (14)
|
1 (<1)
|
|
* Grading based on NCI Common Terminology
for Adverse Events (CTCAE) version 4.0
1 Neutropenia includes febrile neutropenia, neutropenia, and
neutrophil count decreased
2 Thrombocytopenia includes platelet count decreased and
thrombocytopenia
3 Leukopenia includes leukopenia and white blood cell count
decreased
4 Arrhythmia includes bradycardia, sinus arrhythmia, sinus
bradycardia, sinus tachycardia, tachycardia and ventricular extrasystoles
5 Pyrexia includes body temperature increased and pyrexia
6 Infusion-related reaction is a composite term that includes
the term infusion-related reaction and the following events occurring with
the first 48 hours of infusion and the event lasted ≤ 2 days: cytokine
release syndrome, eye swelling, hypertension, hypotension, myalgia,
periorbital edema, pruritus generalized, pyrexia, and rash
7 Decreased immunoglobulins includes blood immunoglobulin A
decreased, blood immunoglobulin G decreased, blood immunoglobulin M
decreased, hypogammaglobulinemia, hypoglobulinemia, and immunoglobulins
decreased
8 Hypertransaminasemia includes alanine aminotransferase
increased, aspartate aminotransferase increased, and hepatic enzyme increased
9 Tremor includes essential tremor, intention tremor, and
tremor
10 Encephalopathy includes cognitive disorder, depressed
level of consciousness, disturbance in attention, encephalopathy, lethargy,
leukoencephalopathy, memory impairment, somnolence, and toxic encephalopathy
11 Insomnia includes initial insomnia, insomnia, and terminal
insomnia
12 Rash includes dermatitis contact, eczema, erythema, rash,
and rash maculopapular
|
Additional adverse reactions in patients with MRD-positive
ALL that did not meet the threshold criteria for inclusion in Table 9 were:
Blood and lymphatic system disorders: anemia
General disorders and administration site
conditions: edema peripheral, pain, and chest pain (includes chest pain
and musculoskeletal chest pain)
Hepatobiliary disorders: blood bilirubin increased
Immune system disorders: hypersensitivity and cytokine
release syndrome
Infections and infestations: viral infectious
disorders, bacterial infectious disorders, and fungal infectious disorders
Injury, poisoning and procedural
complications: medication error and overdose (includes overdose and
accidental overdose)
Investigations: blood alkaline phosphatase increased
Musculoskeletal and connective tissue disorders: pain
in extremity and bone pain
Nervous system disorders: seizure (includes seizure
and generalized tonic-clonic seizure), speech disorder, and hypoesthesia
Psychiatric disorders: confusional state,
disorientation, and depression
Respiratory, thoracic and mediastinal
disorders: dyspnea and productive cough
Vascular disorders: hypertension (includes blood
pressure increased and hypertension) flushing (includes flushing and hot
flush), and capillary leak syndrome
PhiladelphiaChromosome-negative Relapsed Or Refractory B-cell
Precursor ALL
The safety data described below reflect exposure to
BLINCYTO in a randomized, open-label, active-controlled clinical study (TOWER
Study) in which 376 patients withPhiladelphiachromosome-negative relapsed or refractory B-cell precursor ALL were treated
with BLINCYTO (n = 267) or standard of care (SOC) chemotherapy (n = 109). The
median age of BLINCYTO-treated patients was 37 years (range: 18 to 80 years),
60% were male, 84% were White, 7% Asian, 2% were Black or African American, 2%
were American Indian or Alaska Native, and 5% were Multiple/Other.
The most common adverse reactions (≥ 20%) in the BLINCYTO
arm were infections (bacterial and pathogen unspecified), pyrexia, headache,
infusion-related reactions, anemia, febrile neutropenia, thrombocytopenia, and
neutropenia. Serious adverse reactions were reported in 62% of patients. The
most common serious adverse reactions (≥ 2%) included febrile neutropenia,
pyrexia, sepsis, pneumonia, overdose, septic shock, CRS, bacterial sepsis,
device related infection, and bacteremia. Adverse reactions of Grade 3 or
higher were reported in 87% of patients. Discontinuation of therapy due to
adverse reactions occurred in 12% of patients treated with BLINCYTO; neurologic
events and infections were the most frequently reported reasons for
discontinuation of treatment due to an adverse reaction. Fatal adverse events
occurred in 16% of patients. The majority of the fatal events were infections.
The adverse reactions occurring at a ≥ 10% incidence for
any grade or ≥ 5% incidence for Grade 3 or higher in the BLINCYTO-treated
patients in first cycle of therapy are summarized in Table 10.
Table 10: Adverse
Reactions Occurring at ≥ 10% Incidence for Any Grade or ≥ 5% Incidence for
Grade 3 or Higher in BLINCYTO-treated Patients in First Cycle of Therapy
|
Adverse Reaction
|
BLINCYTO
(N = 267)
|
Standard of Care (SOC)
Chemotherapy
(N = 109)
|
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
|
Blood and lymphatic system disorders
|
|
Neutropenia1
|
84 (31)
|
76 (28)
|
67 (61)
|
61 (56)
|
|
Anemia2
|
68 (25)
|
52 (19)
|
45 (41)
|
37 (34)
|
|
Thrombocytopenia3
|
57 (21)
|
47 (18)
|
42 (39)
|
40 (37)
|
|
Leukopenia4
|
21 (8)
|
18 (7)
|
9 (8)
|
9 (8)
|
|
Cardiac disorders
|
|
Arrhythmia5
|
37 (14)
|
5 (2)
|
18 (17)
|
0 (0)
|
|
General disorders and administration site
conditions
|
|
Pyrexia
|
147 (55)
|
15 (6)
|
43 (39)
|
4 (4)
|
|
Edema6
|
48 (18)
|
3 (1)
|
20 (18)
|
1 (1)
|
|
Immune system disorders
|
|
Cytokine release syndrome7
|
37 (14)
|
8 (3)
|
0 (0)
|
0 (0)
|
|
Infections and infestations
|
|
Infections - pathogen unspecified
|
74 (28)
|
40 (15)
|
50 (46)
|
35 (32)
|
|
Bacterial infectious disorders
|
38 (14)
|
19 (7)
|
35 (32)
|
21 (19)
|
|
Viral infectious disorders
|
30 (11)
|
4 (1)
|
14 (13)
|
0 (0)
|
|
Fungal infectious disorders
|
27 (10)
|
13 (5)
|
15 (14)
|
9 (8)
|
|
Injury, poisoning and procedural
complications
|
|
Infusion-related reaction8
|
79 (30)
|
9 (3)
|
9 (8)
|
1 (1)
|
|
Investigations
|
|
Hypertransaminasemia9
|
40 (15)
|
22 (8)
|
13 (12)
|
7 (6)
|
|
Nervous system disorders
|
|
Headache
|
61 (23)
|
1 (<1)
|
30 (28)
|
3 (3)
|
|
Skin and subcutaneous tissue disorders
|
|
Rash10
|
31 (12)
|
2 (1)
|
21 (19)
|
0 (0)
|
|
* Grading based on NCI Common Terminology
Criteria for Adverse Events (CTCAE) version 4.0
1 Neutropenia includes agranulocytosis, febrile neutropenia,
neutropenia, and neutrophil count decreased
2 Anemia includes anemia and hemoglobin decreased
3 Thrombocytopenia includes platelet count decreased and
thrombocytopenia
4 Leukopenia includes leukopenia and white blood cell count
decreased
5 Arrhythmia includes arrhythmia, atrial fibrillation, atrial
flutter, bradycardia, sinus bradycardia, sinus tachycardia, supraventricular
tachycardia, and tachycardia
6 Edema includes face edema, fluid retention, edema, edema
peripheral, peripheral swelling, and swelling face
7 Cytokine release syndrome includes cytokine release syndrome
and cytokine storm
8 Infusion-related reaction is a composite term that includes
the term infusion-related reaction and the following events occurring with
the first 48 hours of infusion and the event lasted ≤ 2 days: pyrexia,
cytokine release syndrome, hypotension, myalgia, acute kidney injury,
hypertension, and rash erythematous
9 Hypertransaminasemia includes alanine aminotransferase
increased, aspartate aminotransferase increased, hepatic enzyme increased,
and transaminases increased
10 Rash includes erythema, rash, rash erythematous, rash generalized,
rash macular, rash maculo-papular, rash pruritic, skin exfoliation, and toxic
skin eruption.
|
Selected laboratory abnormalities worsening from baseline
Grade 0-2 to treatment-related maximal Grade 3-4 in first cycle of therapy are
shown in Table 11.
Table 11: Selected
Laboratory Abnormalities Worsening from Baseline Grade 0-2 to Treatment-related
Maximal Grade 3-4* in First Cycle of Therapy
|
|
BLINCYTO Grade 3 or 4 (%)
|
SOC Chemotherapy Grade 3 or 4
(%)
|
|
Hematology
|
|
Decreased lymphocyte count
|
80
|
83
|
|
Decreased white blood cell count
|
53
|
97
|
|
Decreased hemoglobin
|
29
|
43
|
|
Decreased neutrophil count
|
57
|
68
|
|
Decreased platelet count
|
47
|
85
|
|
Chemistry
|
|
Increased ALT
|
11
|
11
|
|
Increased bilirubin
|
5
|
4
|
|
Increased AST
|
8
|
4
|
|
* Includes only patients who had both baseline
and at least one laboratory measurement during first cycle of therapy
available.
|
Relapsed Or Refractory B-cell
Precursor ALL
Other important adverse reactions from pooled relapsed or
refractory B-cell precursor ALL studies were:
Blood and lymphatic system disorders: lymphadenopathy, hematophagic histiocytosis, and leukocytosis (includes leukocytosis and
white blood cell count increased)
General disorders and administration site
conditions: chills, chest pain (includes chest discomfort, chest pain,
musculoskeletal chest pain, and non-cardiac chest pain), pain, body temperature
increased, hyperthermia, and systemic inflammatory response syndrome
Hepatobiliary disorders: hyperbilirubinemia (includes blood
bilirubin increased and hyperbilirubinemia)
Immune system disorders: hypersensitivity (includes
hypersensitivity, anaphylactic reaction, angioedema, dermatitis allergic, drug eruption, drug
hypersensitivity, erythema multiforme, and urticaria)
Injury, poisoning and procedural
complications: medication error and overdose (includes overdose,
medication error, and accidental overdose)
Investigations: weight increased, decreased
immunoglobulins (includes immunoglobulins decreased, blood immunoglobulin A decreased, blood immunoglobulin G decreased, blood immunoglobulin M decreased, and
hypogammaglobulinemia), blood alkaline phosphatase increased, and
hypertransaminasemia
Metabolism and nutrition disorders: tumor lysis
syndrome
Musculoskeletal and connective tissue disorders: back pain, bone pain, and pain in extremity
Nervous system disorders: tremor (resting tremor,
intention tremor, essential tremor, and tremor), altered state
of consciousness (includes altered state of consciousness, depressed level of
consciousness, disturbance in attention, lethargy, mental status changes, stupor,
and somnolence), dizziness, memory impairment,
seizure (includes seizure, and atonic seizure), aphasia, cognitive disorder, speech disorder, hypoesthesia, encephalopathy,
and cranial nerve disorders (trigeminal neuralgia, trigeminal nerve disorder, sixth
nerve paralysis, cranial nerve disorder, facial nerve disorder, and facial paresis).
Psychiatric disorders: insomnia, disorientation,
confusional state, and depression (includes depressed mood, depression,
suicidal ideation, and completed suicide)
Respiratory, thoracic and mediastinal disorders: dyspnea (includes acute respiratory failure, dyspnea, dyspnea
exertional, respiratory failure, respiratory distress, bronchospasm, bronchial
hyperreactivity, tachypnea, and wheezing), cough, and productive cough
Vascular disorders: hypotension (includes blood pressure
decreased, hypotension, hypovolemic shock, and circulatory collapse), hypertension (includes blood pressure
increased, hypertension, and hypertensive crisis), flushing (includes
flushing and hot flush), and capillary leak syndrome
Postmarketing Experience
The following adverse reactions have been identified during
postapproval use of BLINCYTO. Because these reactions are reported voluntarily
from a population of uncertain size, it is not always possible to reliably
estimate their frequency or establish a causal relationship to drug exposure.
· Fatal pancreatitis has been
reported in patients receiving BLINCYTO in combination with dexamethasone
[see WARNINGS AND PRECAUTIONS].
Immunogenicity
As with all therapeutic proteins, there is potential for
immunogenicity. The immunogenicity of BLINCYTO has been evaluated using either
an electrochemiluminescence detection technology (ECL) or an enzyme-linked immunosorbent assay (ELISA) screening immunoassay for the detection
of binding anti-blinatumomab antibodies. For patients whose sera tested
positive in the screening immunoassay, an in vitro biological assay was
performed to detect neutralizing antibodies.
In clinical studies, less than 2% of patients treated with
BLINCYTO tested positive for binding anti-blinatumomab antibodies. Of patients
who developed anti-blinatumomab antibodies, 7 out of 9 (78%) had in vitro
neutralizing activity. Anti-blinatumomab antibody formation may affect
pharmacokinetics of BLINCYTO.
If formation of anti-blinatumomab antibodies with a
clinically significant effect is suspected, contact Amgen at 1-800-77-AMGEN
(1-800-772-6436) to discuss antibody testing.
The detection of anti-blinatumomab antibody formation is
highly dependent on the sensitivity and specificity of the assay. Additionally,
the observed incidence of antibody (including neutralizing antibody) positivity
in an assay may be influenced by several factors, including assay methodology,
sample handling, timing of sample collection, concomitant medications, and
underlying disease. For these reasons, comparison of the incidence of
antibodies to blinatumomab with the incidence of antibodies to other products
may be misleading.
DRUG INTERACTIONS
No formal drug interaction studies have been conducted with
BLINCYTO. Initiation of BLINCYTO treatment causes transient release of
cytokines that may suppress CYP450 enzymes. The highest drug-drug interaction
risk is during the first 9 days of the first cycle and the first 2 days of the
second cycle in patients who are receiving concomitant CYP450 substrates,
particularly those with a narrow therapeutic index. In these patients, monitor
for toxicity (eg, warfarin) or drug concentrations (eg, cyclosporine). Adjust the dose of the
concomitant drug as needed [see CLINICAL
PHARMACOLOGY].
Warnings
& Precautions
WARNINGS
Included as part of the PRECAUTIONS section.
PRECAUTIONSCytokine Release Syndrome
Cytokine Release Syndrome (CRS), which may be life-threatening
or fatal, occurred in patients receiving BLINCYTO. The median time to onset of
CRS was 2 days after the start of infusion. Manifestations of CRS include
fever, headache, nausea, asthenia, hypotension, increased alanine aminotransferase, increased aspartate aminotransferase, increased total
bilirubin, and disseminated intravascular coagulation (DIC). The manifestations of
CRS after treatment with BLINCYTO overlap with those of infusion reactions,
capillary leak syndrome (CLS), and hemophagocytic histiocytosis/macrophage activation syndrome (MAS).
Using all of these terms to define CRS in clinical trials of BLINCYTO, CRS was
reported in 15% of patients with relapsed or refractory ALL and in 7% of
patients with MRD-positive ALL.
Monitor patients for signs or symptoms of these events.
Advise outpatients on BLINCYTO to contact their healthcare professional for
signs and symptoms associated with CRS. If severe CRS occurs, interrupt
BLINCYTO until CRS resolves. Discontinue BLINCYTO permanently if
life-threatening CRS occurs [see DOSAGE
AND ADMINISTRATION].
Neurological Toxicities
In patients with ALL receiving BLINCYTO in clinical
studies, neurological toxicities have occurred in approximately 65% of
patients. Among patients that experienced a neurologic event, the median time
to the first event was within the first 2 weeks of BLINCYTO treatment and the
majority of events resolved. The most common (≥ 10%) manifestations of
neurological toxicity were headache, and tremor; the neurological toxicity
profile varied by age group [see Use In Specific Populations]. Grade 3 or
higher (severe, life-threatening, or fatal) neurological toxicities following
initiation of BLINCYTO administration occurred in approximately 13% of patients
and included encephalopathy, convulsions, speech disorders, disturbances in
consciousness, confusion and disorientation, and coordination and balance
disorders. Manifestations of neurological toxicity included cranial nerve
disorders. The majority of neurologic events resolved following interruption of
BLINCYTO, but some resulted in treatment discontinuation.
There is limited experience with BLINCYTO in patients with
active ALL in the central nervous system (CNS) or a history
of neurologic events. Patients with a history or presence of clinically relevant
CNS pathology were excluded from clinical
studies.
Monitor patients receiving BLINCYTO for signs and symptoms
of neurological toxicities. Advise outpatients on BLINCYTO to contact their
healthcare professional if they develop signs or symptoms of neurological
toxicities. Interrupt or discontinue BLINCYTO as recommended [see DOSAGE
AND ADMINISTRATION].
Infections
In patients with ALL receiving BLINCYTO in clinical
studies, serious infections such as sepsis, pneumonia, bacteremia, opportunistic infections,
and catheter-site infections were observed in
approximately 25% of patients, some of which were life-threatening or fatal. As
appropriate, administer prophylactic antibiotics and employ
surveillance testing during treatment with BLINCYTO. Monitor patients for signs
and symptoms of infection and treat appropriately.
Tumor Lysis Syndrome
Tumor lysis syndrome (TLS), which may be life-threatening
or fatal, has been observed in patients receiving BLINCYTO. Appropriate
prophylactic measures, including pretreatment nontoxic cytoreduction and
on-treatment hydration, should be used for the prevention of TLS during
BLINCYTO treatment. Monitor for signs or symptoms of TLS. Management of these
events may require either temporary interruption or discontinuation of BLINCYTO
[see DOSAGE AND ADMINISTRATION].
Neutropenia And Febrile
Neutropenia
Neutropenia and febrile neutropenia, including
life-threatening cases, have been observed in patients receiving BLINCYTO.
Monitor laboratory parameters (including, but not limited to, white blood cell count and absolute neutrophil count) during BLINCYTO
infusion. Interrupt BLINCYTO if prolonged neutropenia occurs.
Effects On Ability To Drive And
Use Machines
Due to the potential for neurologic events, including
seizures, patients receiving BLINCYTO are at risk for loss of consciousness
[see Neurological Toxicities]. Advise patients to refrain from driving and
engaging in hazardous occupations or activities such as operating heavy or
potentially dangerous machinery while BLINCYTO is being administered.
Elevated Liver Enzymes
Treatment with BLINCYTO was associated with transient
elevations in liver enzymes. In patients with ALL receiving BLINCYTO in
clinical studies, the median time to onset of elevated liver enzymes was 3
days.
The majority of these transient elevations in liver enzymes
were observed in the setting of CRS. For the events that were observed outside
the setting of CRS, the median time to onset was 19 days. Grade 3 or greater
elevations in liver enzymes occurred in approximately 7% of patients outside
the setting of CRS and resulted in treatment discontinuation in less than 1% of
patients.
Monitor alanine aminotransferase (ALT), aspartate
aminotransferase (AST), gamma-glutamyl transferase (GGT), and total blood
bilirubin prior to the start of and during BLINCYTO treatment. Interrupt
BLINCYTO if the transaminases rise to greater than 5 times the upper limit of
normal or if total bilirubin rises to more than 3 times the upper limit of
normal.
Pancreatitis
Fatal pancreatitis has been reported in patients receiving
BLINCYTO in combination with dexamethasone in clinical studies and the
postmarketing setting [see ADVERSE
REACTIONS].
Evaluate patients who develop signs and symptoms of
pancreatitis. Management of pancreatitis may require either temporary
interruption or discontinuation of BLINCYTO and dexamethasone [see DOSAGE
AND ADMINISTRATION].
Leukoencephalopathy
Cranial magnetic resonance imaging (MRI) changes showing leukoencephalopathy have
been observed in patients receiving BLINCYTO, especially in patients with prior
treatment with cranial irradiation and antileukemic chemotherapy (including systemic
high-dose methotrexate or intrathecal cytarabine).
The clinical significance of these imaging changes is unknown.
Preparation And Administration
Errors
Preparation and administration errors have occurred with
BLINCYTO treatment. Follow instructions for preparation (including admixing)
and administration strictly to minimize medication errors (including underdose
and overdose) [see DOSAGE AND ADMINISTRATION].
Immunization
The safety of immunization with live viral vaccines during or following BLINCYTO
therapy has not been studied. Vaccination with live virus vaccines is
not recommended for at least 2 weeks prior to the start of BLINCYTO treatment,
during treatment, and until immune recovery following last cycle of BLINCYTO.
Risk Of Serious Adverse
Reactions In Pediatric Patients Due To Benzyl Alcohol Preservative
Serious and fatal adverse reactions including “gasping
syndrome” can occur in neonates and infants treated with benzyl
alcohol-preserved drugs, including BLINCYTO (with preservative). The “gasping
syndrome” is characterized by central nervous system depression,
metabolic acidosis, and gasping respirations.
When prescribing BLINCYTO (with preservative) for pediatric
patients, consider the combined daily metabolic load of benzyl alcohol from all
sources including BLINCYTO (with preservative) (contains 7.4 mg of benzyl alcohol per mL) and other drugs
containing benzyl alcohol. The minimum amount of benzyl alcohol at which
serious adverse reactions may occur is not known [see Use In Specific
Populations].
Due to the addition of bacteriostatic saline, 7-day bags of
BLINCYTO solution for infusion with preservative contain benzyl alcohol and are
not recommended for use in any patients weighing less than 22 kg [see DOSAGE
AND ADMINISTRATION and Use In Specific Populations].
Patient Counseling Information
Advise the patient to read the FDA-approved patient
labeling (Medication Guide).
Cytokine Release Syndrome (CRS)
Advise patients of the risk of CRS and infusion reactions,
and to contact their healthcare professional for signs and symptoms associated
with CRS or infusion reactions (pyrexia, fatigue, nausea, vomiting, chills,
hypotension, rash, and wheezing) [see WARNINGS AND
PRECAUTIONS and ADVERSE REACTIONS].
Neurological Toxicities
Advise patients of the risk of neurological toxicities, and
to contact their healthcare professional for signs and symptoms associated with
this event (convulsions, speech disorders, and confusion) [see WARNINGS
AND PRECAUTIONS and ADVERSE
REACTIONS].
Infections
Advise patients of the risk of infections, and to contact
their healthcare professional for signs or symptoms of infection
[see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Inform patients of the importance of keeping the skin clean
around the intravenous catheter to reduce the risk of infection.
Pancreatitis
Advise patients of the risk of pancreatitis and to contact
their healthcare provider for signs or symptoms of pancreatitis, which include
severe and persistent stomach pain, with or without nausea and vomiting
[see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Driving And Engaging In Hazardous
Occupations
Advise patients to refrain from driving and engaging in
hazardous occupations or activities such as operating heavy or potentially
dangerous machinery while BLINCYTO is being administered. Patients should be
advised that they may experience neurological events [see WARNINGS AND
PRECAUTIONS].
Infusion Pump Errors
Inform patients they should not adjust the setting on the
infusion pump. Any changes to pump function may result in dosing errors. If
there is a problem with the infusion pump or the pump alarms, patients should
contact their doctor or nurse immediately.
Nonclinical ToxicologyCarcinogenesis, Mutagenesis,
Impairment Of Fertility
No carcinogenicity or genotoxicity studies have been
conducted with blinatumomab.
No studies have been conducted to evaluate the effects of
blinatumomab on fertility. A murine surrogate molecule had no adverse effects
on male and female reproductive organs in a 13-week repeat-dose toxicity study
in mice.
Use In Specific
PopulationsPregnancyRisk Summary
Based on its mechanism of action, BLINCYTO may cause fetal
harm including B-cell lymphocytopenia when administered to a pregnant woman
[see CLINICAL PHARMACOLOGY]. There are no data on
the use of BLINCYTO in pregnant women. In animal reproduction studies, a murine
surrogate molecule administered to pregnant mice crossed the placental barrier
(see Data). Advise pregnant women of the potential risk to a fetus.
The background rate of major birth defects and miscarriage is unknown for the indicated
population. In theU.S.general population, the estimated background risk of major birth defects and
miscarriage in clinically recognized pregnancies is 2-4% and 15-20%,
respectively.
Clinical Considerations
Fetal/Neonatal Adverse Reactions
Due to the potential for B-cell lymphocytopenia in infants
following exposure to BLINCYTO in-utero, the infant's B lymphocytes should be
monitored before the initiation of live virus vaccination [see WARNINGS
AND PRECAUTIONS].
Data
Animal Data
Animal reproduction studies have not been conducted with
blinatumomab. In embryo-fetal developmental toxicity studies, a murine
surrogate molecule was administered intravenously to pregnant mice during the
period of organogenesis. The surrogate molecule crossed the placental barrier
and did not cause embryo-fetal toxicity or teratogenicity. The expected
depletions of B and T cells were observed in the pregnant mice, but
hematological effects were not assessed in fetuses.
LactationRisk Summary
There is no information regarding the presence of
blinatumomab in human milk, the effects on the breastfed infant, or the effects
on milk production. Because many drugs are excreted in human milk and because
of the potential for serious adverse reactions in nursing infants from
BLINCYTO, including B-cell lymphocytopenia, advise patients not to breastfeed
during and for at least 48 hours after treatment with BLINCYTO.
Females And Males Of
Reproductive Potential
Based on its mechanism of action, BLINCYTO may cause fetal
harm when administered to a pregnant woman [see Use In Specific
Populations].
Pregnancy Testing
Verify the pregnancy status of females of reproductive
potential prior to initiating BLINCYTO treatment.
Contraception
Females
Advise females of reproductive potential to use effective
contraception during treatment and for at least 48 hours after the last dose of
BLINCYTO.
Pediatric Use
The safety and efficacy of BLINCYTO have been established
in pediatric patients with relapsed or refractory B-cell precursor ALL. Use of
BLINCYTO is supported by a single-arm trial in pediatric patients with relapsed
or refractory B-cell precursor ALL. This study included pediatric patients in
the following age groups: 10 infants (1 month up to less than 2 years), 40
children (2 years up to less than 12 years), and 20 adolescents (12 years to
less than 18 years). No differences in efficacy were observed between the
different age subgroups. The efficacy has also been established based on
extrapolation from adequate and well-controlled studies in adults with
MRD-positive B-cell precursor ALL.
In general, the adverse reactions in BLINCYTO-treated
pediatric patients were similar in type to those seen in adult patients with
relapsed or refractory B-cell precursor ALL [see ADVERSE
REACTIONS]. Adverse reactions that were observed more frequently (≥
10% difference) in the pediatric population compared to the adult population
were pyrexia (80% vs. 61%), hypertension (26% vs. 8%), anemia (41% vs. 24%), infusion-related
reaction (49% vs. 34%), thrombocytopenia (34% vs. 21%), leukopenia (24% vs. 11%), and weight
increased (17% vs. 6%).
In pediatric patients less than 2 years old (infants), the
incidence of neurologic toxicities was not significantly different than for the
other age groups, but its manifestations were different; the only event terms
reported were agitation, headache, insomnia, somnolence, and irritability.
Infants also had an increased incidence of hypokalemia (50%) compared to other pediatric
age cohorts (15-20%) or adults (17%).
The steady-state concentrations of blinatumomab were
comparable in adult and pediatric patients at the equivalent dose levels based
on BSA-based regimens.
Benzyl Alcohol Toxicity In
Pediatric Patients
Serious adverse reactions including fatal reactions and the
“gasping syndrome” occurred in premature neonates and infants in the neonatal intensive care unit who received
drugs containing benzyl alcohol as a preservative. In these cases, benzyl
alcohol dosages of 99 to 234 mg/kg/day produced high levels of benzyl alcohol
and its metabolites in the blood and urine (blood levels of benzyl alcohol were
0.61 to 1.378 mmol/L). Additional adverse reactions included gradual
neurological deterioration, seizures, intracranial hemorrhage, hematologic
abnormalities, skin breakdown, hepatic and renal failure, hypotension, bradycardia, and cardiovascular collapse. Preterm,
low-birth weight infants may be more likely to develop these reactions because
they may be less able to metabolize benzyl alcohol.
When prescribing BLINCYTO (with preservative) in pediatric
patients, consider the combined daily metabolic load of benzyl alcohol from all
sources including BLINCYTO (with preservative) (contains 7.4 mg of benzyl
alcohol per mL) and other drugs containing benzyl alcohol. The minimum amount
of benzyl alcohol at which serious adverse reactions may occur is not known
[see WARNINGS AND PRECAUTIONS].
Due to the addition of bacteriostatic saline, 7-day bags of
BLINCYTO solution for infusion contain benzyl alcohol and are not recommended
for use in patients weighing less than 22 kg. Prepare BLINCYTO solution for
infusion with preservative-free saline (24- or 48-hour bags) for use in
patients weighing less than 22 kg [see DOSAGE
AND ADMINISTRATION].
Geriatric Use
Of the total number of patients with ALL treated in
clinical studies of BLINCYTO approximately 12% were 65 and over, while 2% were
75 and older. No overall differences in safety or effectiveness were observed
between these patients and younger patients, and other reported clinical
experience has not identified differences in responses between the elderly and
younger patients. However, elderly patients experienced a higher rate of
serious infections and neurological toxicities, including cognitive disorder,
encephalopathy, and confusion [see WARNINGS AND PRECAUTIONS].
Overdosage
& Contraindications
OVERDOSE
Overdoses have been observed, including one adult patient
who received 133-fold the recommended therapeutic dose of BLINCYTO delivered
over a short duration.
In the dose evaluation phase of the Phase ½ study in
pediatric and adolescent patients with relapsed or refractory B-cell precursor
ALL, one patient experienced a fatal cardiac failure event in the setting of
life-threatening cytokine release syndrome (CRS) at a 30 mcg/m²/day (higher
than the maximum tolerated/recommended) dose [see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Overdoses resulted in adverse reactions, which were
consistent with the reactions observed at the recommended therapeutic dose and
included fever, tremors, and headache. In the event of overdose, interrupt the
infusion, monitor the patient for signs of toxicity, and provide supportive care [see WARNINGS
AND PRECAUTIONS]. Consider re-initiation of
BLINCYTO at the correct therapeutic dose when all toxicities have resolved and
no earlier than 12 hours after interruption of the infusion [see DOSAGE
AND ADMINISTRATION].
CONTRAINDICATIONS
BLINCYTO is contraindicated in patients with known
hypersensitivity to blinatumomab or to any component of the product
formulation.
Clinical
Pharmacology
CLINICAL PHARMACOLOGYMechanism Of Action
Blinatumomab is a bispecific CD19-directed CD3 T-cell
engager that binds to CD19 expressed on the surface of cells of B-lineage
origin and CD3 expressed on the surface of T cells. It activates endogenous T cells by connecting CD3 in
the T-cell receptor (TCR) complex with CD19
on benign and malignant B cells. Blinatumomab mediates
the formation of a synapse between the T-cell and the tumor
cell, upregulation of cell adhesion molecules,
production of cytolytic proteins, release of inflammatory cytokines, and
proliferation of T cells, which result in redirected lysis of CD19+ cells.
Pharmacodynamics
During the continuous intravenous infusion over 4 weeks,
the pharmacodynamic response was characterized by T-cell activation and initial
redistribution, reduction in peripheral B cells, and transient cytokine
elevation.
Peripheral T-cell redistribution (ie, T-cell adhesion to
blood vessel endothelium and/or transmigration into
tissue) occurred after start of BLINCYTO infusion or dose escalation. T-cell
counts initially declined within 1 to 2 days and then returned to baseline
levels within 7 to 14 days in the majority of patients. Increase of T-cell
counts above baseline (T-cell expansion) was observed in few patients.
Peripheral B cell counts decreased to less than or
equal to 10 cells/microliter during the first treatment cycle at doses ≥ 5
mcg/m²/day or ≥ 9 mcg/day in the majority of patients. No recovery of
peripheral B-cell counts was observed during the 2-week BLINCYTO-free period between
treatment cycles. Incomplete depletion of B cells occurred at doses of 0.5
mcg/m²/day and 1.5 mcg/m²/day and in a few patients at higher doses.
Cytokines including IL-2, IL-4, IL-6, IL-8, IL-10, IL-12, TNF-α, and IFN-γ were measured, and IL-6,
IL-10, and IFN-γ were elevated. The highest elevation of cytokines was observed
in the first 2 days following start of BLINCYTO infusion. The elevated cytokine
levels returned to baseline within 24 to 48 hours during the infusion. In
subsequent treatment cycles, cytokine elevation occurred in fewer patients with
lesser intensity compared to the initial 48 hours of the first treatment cycle.
Pharmacokinetics
The pharmacokinetics of blinatumomab appear linear over a dose
range from 5 to 90 mcg/m²/day (approximately equivalent to 9 to 162 mcg/day) in
adult patients. Following continuous intravenous infusion, the steady-state
serum concentration (Css) was achieved within a day and remained stable over
time. The increase in mean Css values was approximately proportional to the
dose in the range tested. At the clinical doses of 9 mcg/day and 28 mcg/day for
the treatment of relapsed or refractory ALL, the mean (SD) Css was 228 (356)
pg/mL and 616 (537) pg/mL, respectively.
Distribution
The estimated mean (SD) volume of distribution based on
terminal phase (Vz) was 4.35 (2.45) L with continuous intravenous infusion of
blinatumomab.
Metabolism
The metabolic pathway of blinatumomab has not been
characterized. Like other protein therapeutics, BLINCYTO is expected to be
degraded into small peptides and amino acids via catabolic pathways.
Elimination
The estimated mean (SD) systemic clearance with continuous
intravenous infusion in patients receiving blinatumomab in clinical studies was
3.11 (2.98) L/hour. The mean (SD) half-life was 2.10 (1.41) hours. Negligible
amounts of blinatumomab were excreted in the urine at the tested clinical
doses.
Gender, Age, And Body Surface
Area
Results of population pharmacokinetic analyses indicate
that age (0.62 to 80 years of age) and gender do not influence the
pharmacokinetics of blinatumomab. Body surface area (0.4 to 2.70 m²) influences
the pharmacokinetics of blinatumomab, however, the clinical relevance of this
effect is unknown.
Hepatic Impairment
No formal pharmacokinetic studies using BLINCYTO have been
conducted in patients with hepatic impairment.
Renal Impairment
No formal pharmacokinetic studies of blinatumomab have been
conducted in patients with renal impairment.
Pharmacokinetic analyses showed an approximately 2-fold
difference in mean blinatumomab clearance values between patients with moderate
renal impairment (CrCL ranging from 30 to 59 mL/min, N = 21) and normal renal
function (CrCL more than 90 mL/min, N = 215). However, high interpatient
variability was discerned (CV% up to 96.8%), and clearance values in renal
impaired patients were essentially within the range observed in patients with
normal renal function. There is no information available in patients with
severe renal impairment (CrCL less than 30 mL/min) or patients on hemodialysis.
Drug Interactions
Transient elevation of cytokines may suppress CYP450 enzyme
activities [see DRUG INTERACTIONS and Pharmacodynamics].
Specific PopulationsPediatrics
The pharmacokinetics of blinatumomab appear linear over a
dose range from 5 to 30 mcg/m²/day in pediatric patients. At the recommended
doses, the mean (SD) steady-state concentration (Css) values were 162 (179) and
533 (392) pg/mL at 5 and 15 mcg/m²/day doses, respectively. The estimated mean
(SD) volume of distribution (Vz), clearance (CL), and terminal half-life (t½,z)
were 3.14 (2.97) L/m², 1.88 (1.90) L/hour/m², and 2.04 (1.35) hours,
respectively.
Clinical StudiesMRD-positive B-cell Precursor
ALLBLAST Study
The efficacy of BLINCYTO was evaluated in an open-label, multicenter,
single-arm study (BLAST Study) [NCT01207388] that included
patients who were ≥ 18 years of age, had received at least 3 chemotherapy
blocks of standard ALL therapy, were in hematologic complete remission (defined
as < 5% blasts in bone marrow, absolute neutrophil count > 1 Gi/L, platelets
> 100 Gi/L) and had MRD at a level of ≥ 0.1% using an assay with a minimum
sensitivity of 0.01%. BLINCYTO was administered at a constant dose of 15
mcg/m²/day (equivalent to the recommended dosage of 28 mcg/day) intravenously
for all treatment cycles. Patients received up to 4 cycles of treatment. Dose
adjustment was possible in case of adverse events.
The treated population included 86 patients in first or
second hematologic complete remission (CR1 or CR2). The demographics and baseline
characteristics are shown in Table 12. The median number of treatment cycles
was 2 (range: 1 to 4). Following treatment with BLINCYTO, 45 out of 61 (73.8%)
patients in CR1 and 14 out of 25 (56.0%) patients in CR2 underwent allogeneic hematopoietic stem cell transplantation in continuous
hematologic complete remission.
Table 12:
Demographics and Baseline Characteristics in BLAST Study
|
Characteristic
|
BLINCYTO
(N = 86)
|
|
Age
|
|
Median, years (min, max)
|
43 (18,76)
|
|
≥ 65 years, n (%)
|
10 (12)
|
|
Males, n (%)
|
50 (58)
|
|
Race, n (%)
|
|
Asian
|
1 (1)
|
|
Other (mixed)
|
0 (0)
|
|
White
|
76 (88)
|
|
Unknown
|
9 (11)
|
|
Philadelphia chromosome disease status, n (%)
|
|
Positive
|
1 (1)
|
|
Negative
|
85 (99)
|
|
Relapse history, n (%)
|
|
Patients in 1st CR
|
61 (71)
|
|
Patients in 2nd CR
|
25 (29)
|
|
MRD level at baseline*, n (%)
|
|
≥ 10%
|
7 (8)
|
|
≥ 1% and < 10%
|
34 (40)
|
|
≥ 0.1% and < 1%
|
45 (52)
|
|
* Assessed centrally using an assay with
minimum sensitivity of 0.01%
|
Efficacy was based on achievement of undetectable MRD
within one cycle of BLINCYTO treatment and hematological relapse-free survival
(RFS). The assay used to assess MRD response had a sensitivity of 0.01% for 6
patients and < 0.005% for 80 patients. Overall, undetectable MRD was
achieved by 70 patients (81.4%: 95% CI: 71.6%, 89.0%). The median hematological
RFS was 22.3 months. Table 13 shows the MRD response and hematological RFS by
remission number.
Table 13: Efficacy
Results in Patients ≥ 18 Years of Age With MRD-positive B-cell Precursor ALL
(BLAST Study)
|
|
Patients in CR1
(n=61)
|
Patients in CR2
(n=25)
|
|
Complete MRD response1, n (%),
[95% CI]
|
52 (85.2)
[73.8, 93.0]
|
18 (72.0)
[50.6, 87.9]
|
|
Median hematological relapse-free survival2 in
months (range)
|
35.2 (0.4, 53.5)
|
12.3 (0.7, 42.3)
|
|
1 Complete MRD response was defined as the
absence of detectable MRD confirmed in an assay with minimum sensitivity of
0.01%
2 Relapse was defined as either hematological or
extramedullary relapse, secondary leukemia, or death due to any cause;
Includes time after transplantation; Kaplan Meier estimate
|
Undetectable MRD was achieved by 65 of 80 patients (81.3%:
95% CI: 71.0%, 89.1%) with an assay sensitivity of at least 0.005%. The
estimated median hematological RFS among the 80 patients using the higher
sensitivity assay was 24.2 months (95% CI: 17.9, NE).
Relapsed/Refractory B-cell
Precursor ALLTOWER Study
The efficacy of BLINCYTO was compared to standard of care
(SOC) chemotherapy in a randomized, open-label, multicenter study (TOWER Study)
[NCT02013167]. Eligible patients were ≥ 18 years of age with relapsed or
refractory B-cell precursor ALL [> 5% blasts in the bone marrow and
refractory to primary induction therapy or refractory to last therapy,
untreated first relapse with first remission duration < 12 months, untreated
second or later relapse, or relapse at any time after allogeneic hematopoietic
stem cell transplantation (alloHSCT)]. BLINCYTO was administered at 9 mcg/day
on Days 1-7 and 28 mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days
1-28 for Cycles 2-5 in 42-day cycles and for Cycles 6-9 in 84-day cycles. Dose
adjustment was possible in case of adverse events. SOC chemotherapy included
fludarabine, cytarabine arabinoside, and granulocyte colony-stimulating factor
(FLAG); high-dose cytarabine arabinoside (HiDAC); high-dose methotrexate-
(HDMTX) based combination; or clofarabine/clofarabine-based regimens.
There were 405 patients randomized 2:1 to receive BLINCYTO
or investigator-selected SOC chemotherapy. Randomization was stratified by age
(< 35 years vs. ≥ 35 years of age), prior salvage therapy (yes vs. no), and
prior alloHSCT (yes vs. no) as assessed at the time of consent. The
demographics and baseline characteristics were well-balanced between the two
arms (see Table 14).
Table 14:
Demographics and Baseline Characteristics in TOWER Study
|
Characteristic
|
BLINCYTO
(N = 271)
|
Standard of Care (SOC)
Chemotherapy
(N = 134)
|
|
Age
|
|
Median, years (min, max)
|
37 (18, 80)
|
37 (18, 78)
|
|
< 35 years, n (%)
|
124 (46)
|
60 (45)
|
|
≥ 35 years, n (%)
|
147 (54)
|
74 (55)
|
|
≥ 65 years, n (%)
|
33 (12)
|
15 (11)
|
|
≥ 75 years, n (%)
|
10 (4)
|
2 (2)
|
|
Males, n (%)
|
162 (60)
|
77 (58)
|
|
Race, n (%)
|
|
American Indian orAlaskaNative
|
4 (2)
|
1 (1)
|
|
Asian
|
19 (7)
|
9 (7)
|
|
Black (or African American)
|
5 (2)
|
3 (2)
|
|
Multiple
|
2 (1)
|
0
|
|
Native Hawaiian or Other Pacific Islander
|
1 (0)
|
1 (1)
|
|
Other
|
12 (4)
|
8 (6)
|
|
White
|
228 (84)
|
112 (84)
|
|
Prior salvage therapy
|
171 (63)
|
70 (52)
|
|
Prior alloHSCT1
|
94 (35)
|
46 (34)
|
|
Eastern Cooperative Group Status - n (%)
|
|
0
|
96 (35)
|
52 (39)
|
|
1
|
134 (49)
|
61 (46)
|
|
2
|
41 (15)
|
20 (15)
|
|
Unknown
|
0
|
1 (1)
|
|
Refractory to salvage treatment - n (%)
|
|
Yes
|
87 (32)
|
34 (25)
|
|
No
|
182 (67)
|
99 (74)
|
|
Unknown
|
2 (1)
|
1 (1)
|
|
Maximum of central/local bone marrow
blasts - n (%)
|
|
≤ 5%
|
0
|
0
|
|
> 5 to < 10%
|
9 (3)
|
7 (5)
|
|
10 to < 50%
|
60 (22)
|
23 (17)
|
|
≥ 50%
|
201 (74)
|
104 (78)
|
|
Unknown
|
1 (0)
|
0
|
|
1 alloHSCT = allogeneic hematopoietic stem cell
transplantation
|
Of the 271 patients randomized to the BLINCYTO arm, 267
patients received BLINCYTO treatment. The median number of treatment cycles was
two (range: 1 to 9 cycles); 267 (99%) received Cycles 1-2 (induction), 86 (32%)
received Cycles 3-5 (consolidation), and 27 (10%) received Cycles 6-9
(continued therapy). Of the 134 patients on the SOC arm, 25 dropped out prior
to start of study treatment, and 109 patients received a median of 1 treatment
cycle (range: 1 to 4 cycles).
The determination of efficacy was based on overall survival
(OS). The study demonstrated statistically
significant improvement in OS for patients treated with BLINCYTO as compared to
SOC chemotherapy. See Figure 1 and Table 15 below for efficacy results from the
TOWER Study.
Figure 1:
Kaplan-Meier Curve of Overall Survival in TOWER Study
Table 15: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Negative
Relapsed or Refractory B-cell Precursor ALL (TOWER Study)
|
|
BLINCYTO
(N = 271)
|
SOC Chemotherapy
(N = 134)
|
|
Overall Survival
|
|
Number of deaths (%)
|
164 (61)
|
87 (65)
|
|
Median, months [95% CI]
|
7.7 [5.6, 9.6]
|
4.0 [2.9, 5.3]
|
|
Hazard Ratio [95% CI]1
|
0.71 [0.55, 0.93]
|
|
p-value2
|
0.012
|
|
Overall Response
|
|
CR4/CRh*5, n (%)
[95% CI]
|
115 (42) [37, 49]
|
27 (20) [14, 28]
|
|
Treatment difference [95% CI]
|
22 [13, 31]
|
|
p-value3
|
< 0.001
|
|
CR, n (%) [95% CI]
|
91 (34) [28, 40]
|
21 (16) [10, 23]
|
|
Treatment difference [95% CI]
|
18 [10, 26]
|
|
p-value3
|
< 0.001
|
|
MRD Response6 for CR/CRh*
|
|
n1/n2 (%)7 [95% CI]
|
73/115 (64) [54, 72]
|
14/27 (52) [32, 71]
|
|
1 Based on stratified Cox’s model.
2 The p-value was derived using stratified log rank test.
3 The p-value was derived using Cochran-Mantel-Haenszel test.
4 CR (complete remission) was defined as ≤ 5% blasts in the
bone marrow, no evidence of disease, and full recovery of peripheral blood
counts (platelets > 100,000/microliter and absolute neutrophil counts
[ANC] > 1,000/microliter).
5 CRh* (complete remission with partial hematologic recovery)
was defined as ≤ 5% blasts in the bone marrow, no evidence of disease, and
partial recovery of peripheral blood counts (platelets > 50,000/microliter
and ANC > 500/microliter).
6 MRD (minimum residual disease) response was defined as MRD
by PCR or flow cytometry < 1 x 10-4 (0.01%).
7 n1: number of patients who achieved MRD response and
CR/CRh*; n2: number of patients who achieved CR/CRh* and had a postbaseline
assessment.
|
Study MT103-211
Study MT103-211 [NCT01466179] was an open-label,
multicenter, single-arm study. Eligible patients were ≥ 18 years of age with
Philadelphia chromosome-negative relapsed or refractory B-cell precursor ALL
(relapsed with first remission duration of ≤ 12 months in first salvage or
relapsed or refractory after first salvage therapy or relapsed within 12 months
of alloHSCT, and had ≥ 10% blasts in bone marrow).
BLINCYTO was administered as a continuous intravenous
infusion. The recommended dose for this study was determined to be 9 mcg/day on
Days 1-7 and 28 mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days 1-28
for subsequent cycles. Dose adjustment was possible in case of adverse events.
The treated population included 185 patients who received at least 1 infusion
of BLINCYTO; the median number of treatment cycles was 2 (range: 1 to 5).
Patients who responded to BLINCYTO but later relapsed had the option to be
retreated with BLINCYTO. Among treated patients, the median age was 39 years
(range: 18 to 79 years), 63 out of 185 (34.1%) had undergone HSCT prior to
receiving BLINCYTO, and 32 out of 185 (17.3%) had received more than 2 prior
salvage therapies.
Efficacy was based on the complete remission (CR) rate,
duration of CR, and proportion of patients with an MRD-negative CR/CR with
partial hematological recovery (CR/CRh*) within 2 cycles of treatment with
BLINCYTO. Table 16 shows the efficacy results from this study. The HSCT rate
among those who achieved CR/CRh* was 39% (30 out of 77).
Table 16: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Negative
Relapsed or Refractory B-cell Precursor ALL (Study MT103-211)
|
|
N = 185
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
60 (32.4) [25.7 - 39.7]
|
17 (9.2) [5.4 - 14.3]
|
77 (41.6) [34.4 - 49.1]
|
|
MRD response3
|
|
n1/n2 (%)4
|
48/60 (80.0)
|
10/17 (58.8)
|
58/77 (75.3)
|
|
[95% CI]
|
[67.7 - 89.2]
|
[32.9 - 81.6]
|
[64.2 - 84.4]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.7 (0.46 - 16.5)
|
5.0 (0.13 - 8.8)
|
5.9 (0.13 - 16.5)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of disease, and full recovery of
peripheral blood counts (platelets > 100,000/microliter and absolute
neutrophil counts [ANC] > 1,000/microliter).
2 CRh* (complete remission with partial hematological
recovery) was defined as ≤ 5% of blasts in the bone marrow, no evidence of
disease, and partial recovery of peripheral blood counts (platelets >
50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. Six CR/CRh* responders with missing MRD data
were considered as MRD-nonresponders.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
|
ALCANTARA Study
The efficacy of BLINCYTO for treatment ofPhiladelphiachromosome-positive B-cell
precursor ALL was evaluated in an open-label, multicenter, single-arm study
(ALCANTARA Study) [NCT02000427]. Eligible patients were ≥ 18 years of age withPhiladelphiachromosome-positive B-cell precursor ALL, relapsed or refractory to at least 1
second generation or later tyrosine kinase inhibitor (TKI), or intolerant to
second generation TKI, and intolerant or refractory to imatinib mesylate.
BLINCYTO was administered at 9 mcg/day on Days 1-7 and 28
mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days 1-28 for subsequent
cycles. Dose adjustment was possible in case of adverse events.
The treated population included 45 patients who received at
least one infusion of BLINCYTO; the median number of treatment cycles was 2
(range: 1 to 5). The demographics and baseline characteristics are shown in
Table 17.
Table 17:
Demographics and Baseline Characteristics in ALCANTARA Study
|
Characteristic
|
BLINCYTO
(N = 45)
|
|
Age
|
|
Median, years (min, max)
|
55 (23, 78)
|
|
≥ 65 years and < 75 years, n (%)
|
10 (22)
|
|
≥ 75 years, n (%)
|
2 (4)
|
|
Males, n (%)
|
24 (53)
|
|
Race, n (%)
|
|
Asian
|
1 (2)
|
|
Black (or African American)
|
3 (7)
|
|
Other
|
2 (4)
|
|
White
|
39 (87)
|
|
Disease History
|
|
Prior TKI treatment1, n (%)
|
|
1
|
7 (16)
|
|
2
|
21 (47)
|
|
≥ 3
|
17 (38)
|
|
Prior salvage therapy
|
31 (62)
|
|
Prior alloHSCT2
|
20(44)
|
|
Bone marrow blasts3
|
|
≥ 50% to < 75%
|
6 (13)
|
|
≥ 75%
|
28(62)
|
|
1 Number of patients that failed ponatinib = 23
(51%)
2 alloHSCT = allogeneic hematopoietic stem cell
transplantation
3 centrally assessed
|
Efficacy was based on the complete remission (CR) rate,
duration of CR, and proportion of patients with an MRD-negative CR/CR with
partial hematological recovery (CR/CRh*) within 2 cycles of treatment with
BLINCYTO. Table 18 shows the efficacy results from ALCANTARA Study. Five of the
16 responding (31%) patients underwent allogeneic HSCT in CR/CRh* induced with
BLINCYTO. There were 10 patients with document T315I mutation; four
achieved CR within 2 cycles of treatment with BLINCYTO.
Table 18: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Positive
Relapsed or Refractory B-cell Precursor ALL (ALCANTARA Study)
|
|
N = 45
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
14 (31) [18 - 47]
|
2 (4) [1 - 15]
|
16 (36) [22 - 51]
|
|
MRD response3
|
|
n1/n2 (%)4
|
12/14 (86)
|
2/2 (100)
|
14/16 (88)
|
|
[95% CI]
|
[57 - 98]
|
[16, 100]
|
[62 - 98]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.7 (3.6 - 12.0)
|
NE6 (3.7 - 9.0)
|
6.7 (3.6 - 12.0)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of disease, and full recovery of
peripheral blood counts (platelets > 100,000/microliter and absolute
neutrophil counts [ANC] > 1,000/microliter).
2 CRh* (complete remission with partial hematological
recovery) was defined as ≤ 5% of blasts in the bone marrow, no evidence of
disease, and partial recovery of peripheral blood counts (platelets >
50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. Six CR/CRh* responders with missing MRD data were
considered as MRD-nonresponders.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
6 NE = not estimable
|
Study MT103-205
Study MT103-205 [NCT01471782] was an open-label,
multicenter, single-arm study in pediatric patients with relapsed or refractory
B-cell precursor ALL (second or later bone marrow relapse, any marrow relapse
after allogeneic HSCT, or refractory to other treatments, and had > 25%
blasts in bone marrow). BLINCYTO was administered at 5 mcg/m²/day on Days 1-7
and 15 mcg/m²/day on Days 8-28 for Cycle 1, and 15 mcg/m²/day on Days 1-28 for
subsequent cycles. Dose adjustment was possible in case of adverse events.
Patients who responded to BLINCYTO but later relapsed had the option to be
retreated with BLINCYTO.
Among the 70 treated patients, the median age was 8 years
(range: 7 months to 17 years), 40 out of 70 (57.1%) had undergone allogeneic
HSCT prior to receiving BLINCYTO, and 39 out of 70 (55.7%) had refractory
disease. The median number of treatment cycles was 1 (range: 1 to 5).
Twenty-three out of 70 (32.9%) patients achieved CR/CRh*
within the first 2 treatment cycles with 17 out of 23 (73.9%) occurring within
Cycle 1 of treatment. See Table 19 for the efficacy results from the study. The
HSCT rate among those who achieved CR/CRh* was 48% (11 out of 23).
Table 19: Efficacy
Results in Patients < 18 Years of Age With Relapsed or Refractory B-cell
Precursor ALL (Study MT103-205)
|
|
N = 70
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
12 (17.1)
[9.2 - 28.0]
|
11 (15.7)
[8.1 - 26.4]
|
23 (32.9)
[22.1 - 45.1]
|
|
MRD response3
|
|
n1/n2 (%)4[95% CI]
|
6/12 (50.0)
[21.1 - 78.9]
|
4/11 (36.4)
[10.9 - 69.2]
|
10/23 (43.5)
[23.2 - 65.5]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.0 (0.5 - 12.1)
|
3.5 (0.5 - 16.4)
|
6.0 (0.5 - 16.4)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of circulating blasts or
extra-medullary disease, and full recovery of peripheral blood counts
(platelets > 100,000/microliter and absolute neutrophil counts [ANC] >
1,000/microliter).
2 CRh* (complete remission with partial hematological recovery)
was defined as ≤ 5% of blasts in the bone marrow, no evidence of circulating
blasts or extra-medullary disease, and partial recovery of peripheral blood
counts (platelets > 50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR or flow cytometry < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. One CR/CRh* responder with missing MRD data was
considered as a MRD-nonresponder.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
|
Medication
Guide
PATIENT INFORMATION
BLINCYTO®
(blin sye' toe)
(blinatumomab) for injection
What is the most important information I should know about
BLINCYTO?
Call your healthcare provider or get emergency medical help
right away if you get any of the symptoms listed below.
BLINCYTO may cause serious side effects that can be severe,
life-threatening, or lead to death, including:
· Cytokine Release Syndrome (CRS)
and Infusion Reactions. Symptoms of CRS and infusion reactions may
include:
o fever
o tiredness or weakness
o dizziness
o headache
o low blood pressure
o nausea
o vomiting
o chills
o face swelling
o wheezing or trouble breathing
o skin rash
· Neurologic
problems. Symptoms of neurologic problems may include:
o seizures
o difficulty in speaking or slurred speech
o loss of consciousness
o trouble sleeping
o confusion and disorientation
o loss of balance
o headache
o difficulty with facial movements, hearing, vision, or swallowing
Your healthcare provider will check for these problems
during treatment with BLINCYTO. Your healthcare provider may temporarily stop
or completely stop your treatment with BLINCYTO, if you have severe side
effects.
See “What are the possible side effects of
BLINCYTO?” below for other side effects of BLINCYTO.
What is BLINCYTO?
BLINCYTO is a prescription medicine used to treat adults
and children with:
· B-cell precursor acute
lymphoblastic leukemia (ALL) in remission with molecular evidence of leukemia
· B-cell precursor ALL that has
come back or did not respond to previous treatments
ALL is a cancer of the blood in which a particular kind of
white blood cell is growing out of control.
Who should not receive BLINCYTO?
Do not receive BLINCYTO if you are allergic to blinatumomab
or to any of the ingredients of BLINCYTO. See the end of this Medication Guide
for a complete list of ingredients in BLINCYTO.
Before receiving BLINCYTO, tell your healthcare provider
about all of your medical conditions, including if you or your child:
· have a history of neurological
problems, such as seizures, confusion, trouble speaking or loss of balance
· have an infection
· have ever had an infusion
reaction after receiving BLINCYTO or other medications
· have a history of radiation treatment to the brain, or
chemotherapy treatment
· are scheduled to receive a
vaccine. You should not receive a “live vaccine” within 2 weeks before you
start treatment with BLINCYTO, during treatment, and until your immune system recovers after you receive
your last cycle of BLINCYTO. If you are not sure about the type of vaccine, ask
your healthcare provider.
· are pregnant or plan to become
pregnant. BLINCYTO may harm your unborn baby. Tell your healthcare provider if
you become pregnant during treatment with BLINCYTO.
o If you are able to become pregnant, your healthcare provider should
do a pregnancy test before you start treatment with BLINCYTO.
o Females who are able to become pregnant should use an effective form
of birth control during treatment with BLINCYTO, and for at least 48 hours
after the last dose of BLINCYTO.
· are breastfeeding or plan to
breastfeed. It is not known if BLINCYTO passes into your breast milk. You
should not breastfeed during treatment with BLINCYTO and for at least 48 hours
after your last treatment.
Tell your healthcare provider about all the medicines you
take, including prescription and over-the-counter medicines, vitamins, and
herbal supplements.
How will I receive BLINCYTO?
· BLINCYTO will be given to you
by intravenous (IV) infusion into your vein by an infusion pump.
· Your healthcare provider will
decide the number of treatment cycles of BLINCYTO.
o You will receive BLINCYTO by continuous IV infusion for 4 weeks (28
days), followed by a 2 week (14 days) break during which you will not receive
BLINCYTO. This is 1 treatment cycle (42 days).
· Your healthcare provider may
prescribe continued therapy.
o You will receive BLINCYTO by continuous IV infusion for 4 weeks (28
days), followed by an 8 week (56 days) break during which you will not receive
BLINCYTO. This is 1 treatment cycle (84 days).
· Your healthcare provider may
give you BLINCYTO in a hospital or clinic for the first 3 to 9 days of the
first treatment cycle and for the first 2 days of the second cycle to check you
for side effects. If you receive additional treatment cycles of BLINCYTO or if
your treatment is stopped for a period of time and restarted, you may also be
treated in a hospital or clinic.
· Your healthcare provider may
change your dose of BLINCYTO, delay, or completely stop treatment with BLINCYTO
if you have certain side effects.
· Your healthcare provider will
do blood tests during treatment with BLINCYTO to check you for side effects.
· Before you receive BLINCYTO,
you will be given a corticosteroid medicine to help reduce infusion
reactions.
· It is very important to keep
the area around the IV catheter clean to reduce the risk of getting an
infection. Your healthcare provider will show you how to care for your catheter
site.
· Do not change the settings on
your infusion pump, even if there is a problem with your pump or your pump
alarm sounds. Any changes to your infusion pump settings may cause a dose that
is too high or too low to be given.
Call your healthcare provider or nurse right away if you
have any problems with your pump or your pump alarm sounds.
What should I avoid while receiving BLINCYTO?
Do not drive, operate heavy machinery, or do other
dangerous activities while you are receiving BLINCYTO because BLINCYTO can
cause neurological symptoms, such as dizziness, seizures, and confusion.
What are the possible side effects of BLINCYTO?
BLINCYTO may cause serious side effects, including:
See “What is the most important information I should
know about BLINCYTO?”
· Infections. BLINCYTO may
cause life-threatening infections that may lead to death. Tell your healthcare
provider right away if you develop any signs or symptoms of an infection.
· Low white blood cell counts
(neutropenia). Neutropenia is common with BLINCYTO treatment and may
sometimes be life-threatening. Low white blood cell counts can increase your
risk of infection. Your healthcare provider will do blood tests to check your
white blood cell count during treatment with BLINCYTO. Tell your healthcare
provider right away if you get a fever.
· Abnormal liver blood tests. Your
healthcare provider will do blood tests to check your liver before you start
BLINCYTO and during treatment with BLINCYTO.
· Inflammation of the pancreas
(pancreatitis). Pancreatitis may happen in people treated with BLINCYTO
and corticosteroids. It may be severe and lead to death. Tell your healthcare
provider right away if you have severe stomach-area pain that does not go away.
The pain may happen with or without nausea and vomiting.
The most common side effects of BLINCYTO include:
· infections
· fever
· headache
· low red blood cell count
(anemia)
· low platelet count (thrombocytopenia)
· reactions related to infusion
of the medicine such as face swelling, low blood pressure, and high blood pressure (infusion-related
reactions)
These are not all the possible side effects of BLINCYTO.
Call your doctor for medical advice about side effects. You
may report side effects to FDA at 1-800-FDA-1088.
How should I store BLINCYTO?
Intravenous (IV) bags containing BLINCYTO for infusion will
arrive in a special package.
· Do not open the package.
· Do not freeze the package.
· The package containing BLINCYTO
will be opened by your healthcare provider and stored in the refrigerator at
36°F to 46°F (2°C to 8°C) for up to 8 days.
· Do not throw away (dispose of)
any BLINCYTO in your household trash. Talk with your healthcare provider about
disposal of BLINCYTO and used supplies.
Keep BLINCYTO and all medicines out of reach of children.
General information about safe and effective use of
BLINCYTO
Medicines are sometimes prescribed for purposes other than
those listed in a Medication Guide. Do not use BLINCYTO for a condition for
which it was not prescribed. Do not give BLINCYTO to other people even if they
have the same symptoms that you have. It may harm them. You can ask your
pharmacist or healthcare provider for information about BLINCYTO that is
written for health professionals.
What are the ingredients in BLINCYTO?
Active ingredient: blinatumomab
Inactive ingredients: citric acid monohydrate, lysine
hydrochloride, polysorbate 80, trehalose dihydrate, sodium hydroxide and
preservative-free sterile water for injection.
https://www.rxlist.com/blincyto-drug.htm#medguide
Blincyto 布利妥莫单抗
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关键信息 博纳吐单抗
外文说明
BLINCYTO®
(blinatumomab) for Injection
WARNING
CYTOKINE RELEASE SYNDROME and NEUROLOGICAL TOXICITIES
·
Cytokine
Release Syndrome (CRS), which may be life-threatening or fatal, occurred in
patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended
[see DOSAGE AND
ADMINISTRATION, WARNINGS AND PRECAUTIONS].
·
Neurological
toxicities, which may be severe, life-threatening, or fatal, occurred in
patients receiving BLINCYTO. Interrupt or discontinue BLINCYTO as recommended
[see DOSAGE AND
ADMINISTRATION, WARNINGS AND PRECAUTIONS].
DESCRIPTION
BLINCYTO
(blinatumomab) is a bispecific CD19-directed CD3 T-cell engager that binds to
CD19 (expressed on cells of B-lineage origin) and CD3 (expressed on T cells).
BLINCYTO is produced in Chinese hamster ovary cells. It consists of 504 amino acids and has a molecular weight of
approximately 54 kilodaltons.
Each
BLINCYTO package contains 1 vial BLINCYTO and 1 vial IV Solution Stabilizer.
BLINCYTO
is supplied in a single-dose vial as a sterile, preservative-free, white to
off-white lyophilized powder for intravenous administration. Each single-dose
vial of BLINCYTO contains 35 mcg blinatumomab, citric acid monohydrate (3.35
mg), lysine hydrochloride (23.23 mg),
polysorbate 80 (0.64 mg), trehalose dihydrate (95.5 mg), and sodium hydroxide
to adjust pH to 7.0. After reconstitution with 3 mL of preservative-free
Sterile Water for Injection, USP, the resulting concentration is 12.5 mcg/mL
blinatumomab.
IV
Solution Stabilizer is supplied in a single-dose vial as a sterile,
preservative-free, colorless to slightly yellow, clear solution. Each
single-dose vial of IV Solution Stabilizer contains citric acid monohydrate
(52.5 mg), lysine hydrochloride (2283.8 mg), polysorbate 80 (10 mg), sodium
hydroxide to adjust pH to 7.0, and water for injection.
INDICATIONSMRD-positive B-cell Precursor ALL
BLINCYTO
is indicated for the treatment of B-cell precursor acute lymphoblastic leukemia (ALL) in
first or second complete remission with minimal residual disease (MRD) greater than or equal to 0.1% in adults
and children.
This
indication is approved under accelerated approval based on MRD response rate
and hematological relapse-free survival. Continued approval for this indication
may be contingent upon verification and description of clinical benefit in the
confirmatory trials.
Relapsed Or Refractory B-cell Precursor ALL
BLINCYTO
is indicated for the treatment of relapsed or refractory B-cell precursor acute
lymphoblastic leukemia (ALL) in adults and children.
DOSAGE AND
ADMINISTRATIONTreatment Of MRD-Positive B-cell Precursor ALL
·
A treatment course consists of 1 cycle of BLINCYTO for induction
followed by up to 3 additional cycles for consolidation.
·
A single cycle of treatment of BLINCYTO induction or
consolidation consists of 28 days of continuous intravenous infusion followed
by a 14-day treatment-free interval (total 42 days).
·
See Table 1 for the recommended dose by patient weight and
schedule. Patients greater than or equal to 45 kg receive a fixed-dose. For
patients less than 45 kg, the dose is calculated using the patient's body
surface area (BSA).
Table 1: Recommended BLINCYTO Dosage and
Schedule for the Treatment of MRD-positive B-cell Precursor ALL
|
Cycle
|
Patient Weight Greater Than or
Equal to 45 kg (Fixed-dose)
|
Patient Weight Less Than 45 kg
(BSA-based dose)
|
|
Induction Cycle 1
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Consolidation Cycles 2-4
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
·
Hospitalization is recommended for the first 3 days of the first
cycle and the first 2 days of the second cycle. For all subsequent cycle starts
and re-initiations (e.g., if treatment is interrupted for 4 or more hours),
supervision by a healthcare professional or hospitalization is recommended.
·
Premedicate with prednisone or equivalent for MRD-positive
B-cell Precursor ALL
o For adult
patients, premedicate with prednisone 100 mg intravenously or equivalent
(e.g., dexamethasone 16 mg) 1 hour prior to the
first dose of BLINCYTO in each cycle.
o For pediatric
patients, premedicate with 5 mg/m² of dexamethasone, to a maximum dose of 20 mg
prior to the first dose of BLINCYTO in the first cycle and when restarting an
infusion after an interruption of 4 or more hours in the first cycle.
·
For administration of BLINCYTO:
o See Section
2.5 for infusion over 24 hours or 48 hours.
o See Section
2.6 for infusion over 7 days using Bacteriostatic 0.9% Sodium Chloride
Injection, USP (containing 0.9% benzyl alcohol). This option is available for
patients weighing greater than or equal to 22 kg. It is not recommended for use
in patients weighing less than 22 kg.
Treatment Of Relapsed Or Refractory B-cell Precursor ALL
·
A treatment course consists of up to 2 cycles of BLINCYTO for
induction followed by 3 additional cycles for consolidation and up to 4 additional
cycles of continued therapy.
·
A single cycle of treatment of BLINCYTO induction or
consolidation consists of 28 days of continuous intravenous infusion followed
by a 14-day treatment-free interval (total 42 days).
·
A single cycle of treatment of BLINCYTO continued therapy
consists of 28 days of continuous intravenous infusion followed by a 56-day
treatment-free interval (total 84 days).
·
See Table 2 for the recommended dose by patient weight and
schedule. Patients greater than or equal to 45 kg receive a fixed-dose and for
patients less than 45 kg, the dose is calculated using the patient's body
surface area (BSA).
Table 2: Recommended BLINCYTO Dosage and
Schedule for the Treatment of Relapsed or Refractory B-cell Precursor ALL
|
Cycle
|
Patient Weight Greater Than or
Equal to 45 kg (Fixed-dose)
|
Patient Weight Less Than 45 kg
(BSA-based dose)
|
|
Induction Cycle 1
|
|
Days 1-7
|
9 mcg/day
|
5 mcg/m²/day (not to exceed 9 mcg/day)
|
|
Days 8-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Induction Cycle 2
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Consolidation Cycles 3-5
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-42
|
14-day treatment-free interval
|
14-day treatment-free interval
|
|
Continued Therapy Cycles 6-9
|
|
Days 1-28
|
28 mcg/day
|
15 mcg/m²/day (not to exceed 28 mcg/day)
|
|
Days 29-84
|
56-day treatment-free interval
|
56-day treatment-free interval
|
·
Hospitalization is recommended for the first 9 days of the first
cycle and the first 2 days of the second cycle. For all subsequent cycle starts
and re-initiation (e.g., if treatment is interrupted for 4 or more hours),
supervision by a healthcare professional or hospitalization is recommended.
·
Premedicate with dexamethasone.
o For adult
patients, premedicate with 20 mg dexamethasone 1 hour prior to the first dose
of BLINCYTO of each cycle, prior to a step dose (such as Cycle 1 Day 8), and
when restarting an infusion after an interruption of 4 or more hours.
o For pediatric
patients, premedicate with 5 mg/m² of dexamethasone, to a maximum dose of 20 mg
prior to the first dose of BLINCYTO in the first cycle, prior to a step dose
(such as Cycle 1 Day 8), and when restarting an infusion after an interruption
of 4 or more hours in the first cycle.
·
For administration of BLINCYTO:
o See Section
2.5 for infusion over 24 hours or 48 hours.
o See Section
2.6 for infusion over 7 days using Bacteriostatic 0.9% Sodium Chloride
Injection, USP (containing 0.9% benzyl alcohol). This option is available for
patients weighing greater than or equal to 22 kg. It is not recommended for use
in patients weighing less than 22 kg.
Dosage Adjustments
If
the interruption after an adverse event is no longer than 7 days, continue the
same cycle to a total of 28 days of infusion inclusive of days before and after
the interruption in that cycle. If an interruption due to an adverse event is
longer than 7 days, start a new cycle.
Table 3: Dose Modifications for Toxicity
|
Toxicity
|
Grade*
|
Patients Greater Than or Equal
to 45 kg
|
Patients Less Than 45 kg
|
|
Cytokine Release Syndrome (CRS)
|
Grade 3
|
Withhold BLINCYTO until resolved, then
restart BLINCYTO at 9 mcg/day. Escalate to 28 mcg/day after 7 days if the
toxicity does not recur.
|
Withhold BLINCYTO until resolved, then
restart BLINCYTO at 5 mcg/m²/day. Escalate to 15 mcg/m²/day after 7 days if
the toxicity does not recur.
|
|
|
Grade 4
|
Discontinue BLINCYTO permanently.
|
|
Neurological Toxicity
|
Seizure
|
Discontinue BLINCYTO permanently if more
than one seizure occurs.
|
|
|
Grade 3
|
Withhold BLINCYTO until no more than Grade
1 (mild) and for at least 3 days, then restart BLINCYTO at 9 mcg/day.
Escalate to 28 mcg/day after 7 days if the toxicity does not recur. If the
toxicity occurred at 9 mcg/day, or if the toxicity takes more than 7 days to
resolve, discontinue BLINCYTO permanently.
|
Withhold BLINCYTO until no more than Grade
1 (mild) and for at least 3 days, then restart BLINCYTO at 5 mcg/m²/day.
Escalate to 15 mcg/m²/day after 7 days if the toxicity does not recur. If the
toxicity occurred at 5 mcg/m²/day, or if the toxicity takes more than 7 days
to resolve, discontinue BLINCYTO permanently.
|
|
Toxicity
|
Grade*
|
Patients Greater Than or Equal to 45 kg
|
Patients Less Than 45 kg
|
|
|
Grade 4
|
Discontinue BLINCYTO permanently.
|
|
Other Clinically Relevant Adverse
Reactions
|
Grade 3
|
Withhold BLINCYTO until no more than Grade
1 (mild), then restart BLINCYTO at 9 mcg/day. Escalate to 28 mcg/day after 7
days if the toxicity does not recur. If the toxicity takes more than 14 days
to resolve, discontinue BLINCYTO permanently.
|
Withhold BLINCYTO until no more than Grade
1 (mild), then restart BLINCYTO at 5 mcg/m²/day. Escalate to 15 mcg/m²/day
after 7 days if the toxicity does not recur. If the toxicity takes more than
14 days to resolve, discontinue BLINCYTO permanently.
|
|
|
Grade 4
|
Consider discontinuing BLINCYTO
permanently.
|
|
* Based on the Common Terminology Criteria
for Adverse Events (CTCAE). Grade 3 is severe, and Grade 4 is
life-threatening.
|
Preparation
It
is very important that the instructions for preparation (including admixing)
and administration provided in this section are strictly followed to minimize
medication errors (including underdose and overdose) [see WARNINGS
AND PRECAUTIONS].
BLINCYTO
can be infused over 24 hours (preservative-free) or 48 hours
(preservative-free), or 7 days (with preservative). The choice between these
options for the infusion duration should be made by the treating physician
considering the frequency of the infusion bag changes and the weight of the
patient. The 7-day infusion is not recommended for patients weighing less than
22 kg.
For
preparation, reconstitution, and administration of BLINCYTO:
·
See Section 2.5 for infusion over 24 hours or 48 hours.
·
See Section 2.6 for infusion over 7 days using Bacteriostatic
0.9% Sodium Chloride Injection, USP (containing 0.9% benzyl alcohol). This
option is available for patients weighing greater than or equal to 22 kg. It is
not recommended for patients weighing less than 22 kg.
Call
1-800-77-AMGEN (1-800-772-6436) if you have questions about the reconstitution
and preparation of BLINCYTO.
Aseptic Preparation
Strictly
observe aseptic technique when preparing the
solution for infusion since BLINCYTO vials do not contain antimicrobial preservatives. To prevent
accidental contamination, prepare BLINCYTO according to aseptic standards,
including but not limited to:
·
Prepare BLINCYTO in a USP <797> compliant facility.
·
Prepare BLINCYTO in an ISO Class 5 laminar flow hood or better.
·
Ensure that the admixing area has appropriate environmental
specifications, confirmed by periodic monitoring.
·
Ensure that personnel are appropriately trained in aseptic
manipulations and admixing of oncology drugs.
·
Ensure that personnel wear appropriate protective clothing and
gloves.
·
Ensure that gloves and surfaces are disinfected.
Package Content
1
package BLINCYTO includes 1 vial of BLINCYTO and 1 vial of IV Solution
Stabilizer.
·
Do not use IV Solution Stabilizer for reconstitution of
BLINCYTO. IV Solution Stabilizer is provided with the BLINCYTO package and
is used to coat the IV bag prior to addition of reconstituted BLINCYTO to
prevent adhesion of BLINCYTO to IV bags and IV
tubing.
·
More than 1 package of BLINCYTO may be needed to prepare some of
the prescribed doses.
Incompatibility Information
BLINCYTO
is incompatible with di-ethylhexylphthalate (DEHP) due to the possibility of particle
formation, leading to a cloudy solution.
·
Use polyolefin, PVC DEHP-free, or ethyl vinyl acetate
(EVA) infusion bags/pump cassettes.
·
Use polyolefin, PVC DEHP-free, or EVA IV tubing sets.
24-Hour Or 48-Hour Infusion Of BLINCYTOPreparation Of BLINCYTO Infusion Bag For 24- Or 48-Hour
Infusion
Verify
the prescribed dose and infusion duration for each BLINCYTO infusion bag. To
minimize errors, use the specific volumes described in Tables 4 to 6 to
prepare the BLINCYTO infusion bag.
·
Table 4 for patients weighing greater than or equal to 45 kg
·
Tables 5 and 6 for patients weighing less than 45 kg
Aseptically
add 270 mL 0.9% Sodium Chloride Injection, USP to the IV bag.Aseptically
transfer 5.5 mL IV Solution Stabilizer to the IV bag containing 0.9%
Sodium Chloride Injection, USP. Gently mix the contents of the bag to
avoid foaming. Discard the vial containing the unused IV Solution
Stabilizer.Aseptically
transfer reconstituted BLINCYTO [see Reconstitution of BLINCYTO]
into the IV bag containing 0.9% Sodium Chloride Injection, USP and IV
Solution Stabilizer. Gently mix the contents of the bag to avoid foaming.
o Refer to
Tables 4 to 6 for the specific volume of reconstituted BLINCYTO.
Under
aseptic conditions, attach the IV tubing to the IV bag with the sterile
0.2 micron in-line filter.
o Ensure that
the IV tubing is compatible with the infusion pump.
Remove
air from the IV bag. This is particularly important for use with an
ambulatory infusion pump. Prime the IV tubing only with the prepared
solution for infusion. Do not prime with 0.9% Sodium Chloride Injection,
USP.Store
at 2°C to 8°C if not used immediately [see DOSAGE AND
ADMINISTRATION].
Table 4: For Patients Weighing Greater Than
or Equal to 45 kg: Volumes to Add to IV Bag
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
Reconstituted BLINCYTO
|
|
9 mcg/day
|
24 hours
|
10 mL/hour
|
0.83 mL
|
|
48 hours
|
5 mL/hour
|
1.7 mL
|
|
28 mcg/day
|
24 hours
|
10 mL/hour
|
2.6 mL
|
|
48 hours
|
5 mL/hour
|
5.2 mL*
|
|
* 2 packages of BLINCYTO are needed for
preparation of 28 mcg/day dose infused over 48 hours at a rate of 5 mL/hour.
|
Table 5: For Patients Weighing Less Than 45
kg: Volumes to Add to IV Bag for 5 mcg/m²/day Dose
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
BSA (m²)
|
Reconstituted BLINCYTO
|
|
5 mcg/m²/day
|
24 hours
|
10 mL/hour
|
1.5 - 1.59
|
0.7 mL
|
|
1.4 - 1.49
|
0.66 mL
|
|
1.3 - 1.39
|
0.61 mL
|
|
1.2 - 1.29
|
0.56 mL
|
|
1.1 - 1.19
|
0.52 mL
|
|
1 - 1.09
|
0.47 mL
|
|
0.9 - 0.99
|
0.43 mL
|
|
0.8 - 0.89
|
0.38 mL
|
|
0.7 - 0.79
|
0.33 mL
|
|
0.6 - 0.69
|
0.29 mL
|
|
0.5 - 0.59
|
0.24 mL
|
|
0.4 - 0.49
|
0.2 mL
|
|
5 mcg/m²/day
|
48 hours
|
5 mL/hour
|
1.5 - 1.59
|
1.4 mL
|
|
1.4 - 1.49
|
1.3 mL
|
|
1.3 - 1.39
|
1.2 mL
|
|
1.2 - 1.29
|
1.1 mL
|
|
1.1 - 1.19
|
1 mL
|
|
1 - 1.09
|
0.94 mL
|
|
0.9 - 0.99
|
0.85 mL
|
|
0.8 - 0.89
|
0.76 mL
|
|
0.7 - 0.79
|
0.67 mL
|
|
0.6 - 0.69
|
0.57 mL
|
|
0.5 - 0.59
|
0.48 mL
|
|
0.4 - 0.49
|
0.39 mL
|
Table 6: For Patients Weighing Less Than 45
kg: Volumes to Add to IV Bag for 15 mcg/m²/day Dose
|
0.9% Sodium Chloride
Injection, USP (starting volume)
|
270 mL
|
|
IV Solution Stabilizer
|
5.5 mL
|
|
Dose
|
Infusion Duration
|
Infusion Rate
|
BSA (m²)
|
Reconstituted BLINCYTO
|
|
15 mcg/m²/day
|
24 hours
|
10 mL/hour
|
1.5 - 1.59
|
2.1 mL
|
|
1.4 - 1.49
|
2 mL
|
|
1.3 - 1.39
|
1.8 mL
|
|
1.2 - 1.29
|
1.7 mL
|
|
1.1 - 1.19
|
1.6 mL
|
|
1 - 1.09
|
1.4 mL
|
|
0.9 - 0.99
|
1.3 mL
|
|
0.8 - 0.89
|
1.1 mL
|
|
0.7 - 0.79
|
1 mL
|
|
0.6 - 0.69
|
0.86 mL
|
|
0.5 - 0.59
|
0.72 mL
|
|
0.4 - 0.49
|
0.59 mL
|
|
15 mcg/m²/day
|
48 hours
|
5 mL/hour
|
1.5 - 1.59
|
4.2 mL*
|
|
1.4 - 1.49
|
3.9 mL*
|
|
1.3 - 1.39
|
3.7 mL*
|
|
1.2 - 1.29
|
3.4 mL*
|
|
1.1 - 1.19
|
3.1 mL*
|
|
1 - 1.09
|
2.8 mL
|
|
0.9 - 0.99
|
2.6 mL
|
|
0.8 - 0.89
|
2.3 mL
|
|
0.7 - 0.79
|
2 mL
|
|
0.6 - 0.69
|
1.7 mL
|
|
0.5 - 0.59
|
1.4 mL
|
|
0.4 - 0.49
|
1.2 mL
|
|
* 2 packages of BLINCYTO are needed for
preparation of 15 mcg/m²/day dose infused over 48 hours at a rate of 5
mL/hour for patients with a BSA greater than 1.09 m².
|
Reconstitution Of BLINCYTOAdd
3 mL of preservative-free Sterile Water for Injection, USP by directing
the water along the walls of the BLINCYTO vial and not directly on the
lyophilized powder (resulting in a final BLINCYTO concentration of 12.5
mcg/mL).
o Do not
reconstitute BLINCYTO with IV Solution Stabilizer.
Gently
swirl contents to avoid excess foaming. Do not shake.Visually
inspect the reconstituted solution for particulate matter and
discoloration during reconstitution and prior to infusion. The resulting
solution should be clear to slightly opalescent, colorless to slightly
yellow. Do not use if solution is cloudy or has precipitated.Administration
·
Administer BLINCYTO as a continuous intravenous infusion at a
constant flow rate using an infusion pump. The pump should be programmable,
lockable, non-elastomeric, and have an alarm.
·
Prepared BLINCYTO infusion bags [see DOSAGE AND
ADMINISTRATION] should be infused over 24 hours or 48 hours.
·
The starting volume (270 mL) is more than the volume
administered to the patient (240 mL) to account for the priming of the IV
tubing and to ensure that the patient will receive the full dose of BLINCYTO.
· Infuse BLINCYTO solution according to the
instructions on the pharmacy label on the prepared bag at one of the following
constant infusion rates:
o Infusion rate
of 10 mL/hour for a duration of 24 hours, OR
o Infusion rate
of 5 mL/hour for a duration of 48 hours
·
The BLINCYTO solution must be administered using IV tubing that
contains a sterile, non-pyrogenic, low protein-binding, 0.2 micron in-line
filter.
·
Important Note: Do not flush the BLINCYTO infusion line or
intravenous catheter, especially when changing infusion bags.Flushingwhen changing bags or at completion of infusion can result in excess dosage and
complications thereof. When administering via a multi-lumen venous catheter,
BLINCYTO should be infused through a dedicated lumen.
·
At the end of the infusion, any unused BLINCYTO solution in the
IV bag and IV tubing should be disposed of in accordance with local requirements.
7-Day Infusion Of BLINCYTO Using Bacteriostatic Saline
This
option is not recommended for use in patients weighing less than 22 kg
[see WARNINGS AND PRECAUTIONS and Use
In Specific Populations].
Preparation Of BLINCYTO Infusion Bag For 7-Day Infusion
Verify
the prescribed dose and infusion duration for each BLINCYTO infusion bag. To
minimize errors, use the specific volumes described in Table 7 to prepare the
BLINCYTO infusion bag.
Aseptically
add 90 mL Bacteriostatic 0.9% Sodium Chloride Injection, USP to the empty
IV bag.Aseptically
transfer 2.2 mL IV Solution Stabilizer to the IV bag containing the saline
solution. Gently mix the contents of the bag to avoid foaming.
Discard the vial containing the unused IV Solution Stabilizer.Aseptically
transfer reconstituted BLINCYTO [see Reconstitution of BLINCYTO]
into the IV bag containing the
saline solution and IV Solution
Stabilizer. Gently mix the contents of the bag to avoid foaming.
o Refer to
Table 7 for the specific volume of reconstituted BLINCYTO.
Aseptically
add 0.9% Sodium Chloride Injection, USP to the IV bag to a final volume of
110 mL resulting in 0.74% benzyl alcohol. Gently mix the contents of
the bag to avoid foaming.
o Refer to
Table 7 for the specific volume of 0.9% Sodium Chloride Injection, USP.
Under
aseptic conditions, attach the IV tubing to the IV bag. An in-line filter
is not required for a 7-day bag.
o Ensure that
the IV tubing is compatible with the infusion pump.
Remove
air from the IV bag. This is particularly important for use with an
ambulatory infusion pump. Prime the IV tubing only with the prepared
solution for infusion. Do not prime with 0.9% Sodium Chloride Injection,
USP.Store
at 2°C to 8°C if not used immediately [see Storage Requirements].
Table 7: For 7-Day Infusion: Volumes to Add
to IV Bag for 28 mcg/day and 15 mcg/m²/day; Not Recommended for Patients Less
Than 22 kg
|
Bacteriostatic 0.9% Sodium Chloride
Injection, USP (starting volume)
|
90 mL
|
|
IV Solution Stabilizer
|
2.2 mL
|
|
Reconstituted BLINCYTO
|
Specific volume listed below in table
|
|
Quantity Sufficient (qs) with 0.9% Sodium
Chloride Injection, USP to a Final Volume of 110 mL
|
|
Infusion Duration
|
7 days
|
|
Infusion Rate
|
0.6 mL/hour
|
|
Patient Weight
|
Dose
|
BSA (m²)
|
Number of BLINCYTO Packages
|
Reconstituted BLINCYTO
|
0.9% Sodium Chloride
Injection, USP to qs to a Final Volume of 110 mL
|
|
Greater than or equal to 45 kg
(fixed-dose)
|
28 mcg/day
|
|
6
|
16.8 mL
|
1 mL
|
|
22-45 kg (BSA-based dose)
|
15 mcg/m²/day
|
1.5 - 1.59
|
5
|
14 mL
|
3.8 mL
|
|
1.4 - 1.49
|
5
|
13.1 mL
|
4.7 mL
|
|
1.30 - 1.39
|
5
|
12.2 mL
|
5.6 mL
|
|
1.20 - 1.29
|
5
|
11.3 mL
|
6.5 mL
|
|
1.10 - 1.19
|
4
|
10.4 mL
|
7.4 mL
|
|
1 - 1.09
|
4
|
9.5 mL
|
8.3 mL
|
|
0.9 - 0.99
|
4
|
8.6 mL
|
9.2 mL
|
Reconstitution Of BLINCYTOAdd
3 mL of preservative-free Sterile Water for Injection, USP by directing
the water along the walls of the BLINCYTO vial and not directly on the
lyophilized powder (resulting in a final BLINCYTO concentration of 12.5
mcg/mL).
o Do not
reconstitute BLINCYTO with IV Solution Stabilizer.
Gently
swirl contents to avoid excess foaming. Do not shake.Visually
inspect the reconstituted solution for particulate matter and
discoloration during reconstitution and prior to infusion. The resulting
solution should be clear to slightly opalescent, colorless to slightly
yellow. Do not use if solution is cloudy or has precipitated.Administration
·
Administer BLINCYTO as a continuous intravenous infusion at a
constant flow rate using an infusion pump. The pump should be programmable,
lockable, non-elastomeric, and have an alarm.
·
Prepared BLINCYTO infusion bags [see Preparation of
BLINCYTO Infusion Bag for 7-Day Infusion] should be infused over 7 days.
·
The final volume of infusion solution (110 mL) will be more than
the volume administered to the patient (100 mL) to account for the priming of
the IV tubing and to ensure that the patient will receive the full dose of
BLINCYTO.
·
Infuse BLINCYTO solution according to the instructions on the
pharmacy label on the prepared bag at an infusion rate of 0.6 mL/hour for a
duration of 7 days.
·
Important Note: Do not flush the BLINCYTO infusion line or
intravenous catheter, especially when changing infusion bags.Flushingwhen changing bags or at completion of infusion can result in excess dosage and
complications thereof. When administering via a multi-lumen venous catheter,
BLINCYTO should be infused through a dedicated lumen.
·
At the end of the infusion, any unused BLINCYTO solution in the
IV bag and IV tubing should be disposed of in accordance with local
requirements.
Storage Requirements
The
information in Table 8 indicates the storage time for the reconstituted
BLINCYTO vial and prepared infusion bag.
Store
lyophilized BLINCYTO and IV Solution Stabilizer vials for a maximum of 8 hours
at room temperature in the original carton to protect from light [see HOW
SUPPLIED/Storage And Handling].
Table 8: Storage Time for Reconstituted
BLINCYTO Vial and Prepared BLINCYTO Infusion Bag
|
|
Maximum Storage Time
|
|
Room Temperature 23°C to 27°C
(73°F to 81°F)
|
Refrigerated 2°C to 8°C (36°F
to 46°F)
|
|
Reconstituted BLINCYTO Vial
|
4 hours
|
24 hours
|
|
Prepared BLINCYTO Infusion Bag
(Preservative-Free)
|
48 hours*
|
8 days
|
|
Prepared BLINCYTO Infusion Bag (with
Preservative)
|
7 days*
|
14 days
|
|
* Storage time includes infusion time. If
the prepared BLINCYTO infusion bag is not administered within the time frames
and temperatures indicated, it must be discarded; it should not be
refrigerated again.
|
HOW SUPPLIEDDosage Forms And Strengths
For
injection: 35 mcg of lyophilized powder in a single-dose vial for
reconstitution.
Each BLINCYTO package (NDC 55513-160-01) contains:
·
One BLINCYTO 35 mcg single-dose vial containing a sterile,
preservative-free, white to off-white lyophilized powder and
·
One IV Solution Stabilizer 10 mL single-dose glass vial
containing a sterile, preservative-free, colorless to slightly yellow, clear
solution. Do not use the IV Solution Stabilizer to reconstitute BLINCYTO.
Storage And Handling
Store
BLINCYTO and IV Solution Stabilizer vials in the original package refrigerated
at 2°C to 8°C (36°F to 46°F) and protect from light until time of use. Do not
freeze.
Store
and transport the prepared IV bag containing BLINCYTO solution for infusion at
2°C to 8°C (36°F to 46°F) conditions. Ship in packaging that has been validated
to maintain temperature of the contents at 2°C to 8°C (36°F to 46°F). Do not
freeze.
Side Effects & Drug
Interactions
SIDE EFFECTS
The following adverse reactions are discussed in greater
detail in other sections of the label:
· Cytokine Release Syndrome
[see WARNINGS AND PRECAUTIONS]
· Neurological Toxicities
[see WARNINGS AND PRECAUTIONS]
· Infections [see WARNINGS
AND PRECAUTIONS]
· Tumor Lysis Syndrome [see WARNINGS
AND PRECAUTIONS]
· Neutropenia and Febrile Neutropenia [see WARNINGS
AND PRECAUTIONS]
· Effects on Ability to Drive and
Use Machines [see WARNINGS AND PRECAUTIONS]
· Elevated Liver Enzymes
[see WARNINGS AND PRECAUTIONS]
· Pancreatitis [see WARNINGS AND PRECAUTIONS]
· Leukoencephalopathy
[see WARNINGS AND PRECAUTIONS]
Clinical Trials Experience
Because clinical trials are conducted under widely varying
conditions, adverse reaction rates observed in the clinical trials of a drug
cannot be directly compared to rates in the clinical trials of another drug and
may not reflect the rates observed in practice.
MRD-Positive B-cell Precursor
ALL
The safety of BLINCYTO in patients with MRD-positive B-cell
precursor ALL was evaluated in two single-arm clinical studies in which 137
patients were treated with BLINCYTO. The median age of the study population was 45 years (range: 18
to 77 years).
The most common adverse reactions (≥ 20%) were pyrexia,
infusion related reactions, headache, infections (pathogen unspecified), tremor, and chills. Serious adverse reactions
were reported in 61% of patients. The most common serious adverse reactions (≥
2%) included pyrexia, tremor, encephalopathy, aphasia, lymphopenia, neutropenia, overdose,
device related infection, seizure, and staphylococcal infection. Adverse reactions of
Grade 3 or higher were reported in 64% of patients. Discontinuation of therapy
due to adverse reactions occurred in 17% of patients; neurologic events were
the most frequently reported reasons for discontinuation. There were 2 fatal
adverse events that occurred within 30 days of the end of BLINCYTO treatment (atypical pneumonia and subdural hemorrhage).
Table 9 summarizes the adverse reactions occurring at a ≥
10% incidence for any grade or ≥ 5% incidence for Grade 3 or higher.
Table 9: Adverse
Reactions Occurring at ≥ 10% Incidence for Any Grade or ≥ 5% Incidence for
Grade 3 or Higher in BLINCYTO-Treated Patients with MRD-Positive B-cell
Precursor ALL (N=137)
|
Adverse Reaction
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
|
Blood and lymphatic system disorders
|
|
Neutropenia1
|
21 (15)
|
21 (15)
|
|
Leukopenia2
|
19 (14)
|
13 (9)
|
|
Thrombocytopenia3
|
14 (10)
|
8 (6)
|
|
Cardiac disorders
|
|
Arrhythmia4
|
17 (12)
|
3 (2)
|
|
General disorders and administration site
conditions
|
|
Pyrexia5
|
125 (91)
|
9 (7)
|
|
Chills
|
39 (28)
|
0 (0)
|
|
Infections and infestations
|
|
Infections - pathogen unspecified
|
53 (39)
|
11 (8)
|
|
Injury, poisoning and procedural
complications
|
|
Infusion related reaction6
|
105 (77)
|
7 (5)
|
|
Investigations
|
|
Decreased immunoglobulins7
|
25 (18)
|
7 (5)
|
|
Weight increased
|
14 (10)
|
1 (<1)
|
|
Hypertransaminasemia8
|
13 (9)
|
9 (7)
|
|
Musculoskeletal and connective tissue
disorders
|
|
Back pain
|
16 (12)
|
1 (<1)
|
|
Nervous system disorders
|
|
Headache
|
54 (39)
|
5 (4)
|
|
Tremor9
|
43 (31)
|
6 (4)
|
|
Aphasia
|
16 (12)
|
1 (<1)
|
|
Dizziness
|
14 (10)
|
1 (<1)
|
|
Encephalopathy10
|
14 (10)
|
6 (4)
|
|
Psychiatric disorders
|
|
Insomnia11
|
24 (18)
|
1 (<1)
|
|
Respiratory, thoracic and mediastinal
disorders
|
|
Cough
|
18 (13)
|
0 (0)
|
|
Skin and subcutaneous tissue disorders
|
|
Rash12
|
22 (16)
|
1 (<1)
|
|
Vascular disorders
|
|
Hypotension
|
19 (14)
|
1 (<1)
|
|
* Grading based on NCI Common Terminology
for Adverse Events (CTCAE) version 4.0
1 Neutropenia includes febrile neutropenia, neutropenia, and
neutrophil count decreased
2 Thrombocytopenia includes platelet count decreased and
thrombocytopenia
3 Leukopenia includes leukopenia and white blood cell count
decreased
4 Arrhythmia includes bradycardia, sinus arrhythmia, sinus
bradycardia, sinus tachycardia, tachycardia and ventricular extrasystoles
5 Pyrexia includes body temperature increased and pyrexia
6 Infusion-related reaction is a composite term that includes
the term infusion-related reaction and the following events occurring with
the first 48 hours of infusion and the event lasted ≤ 2 days: cytokine
release syndrome, eye swelling, hypertension, hypotension, myalgia,
periorbital edema, pruritus generalized, pyrexia, and rash
7 Decreased immunoglobulins includes blood immunoglobulin A
decreased, blood immunoglobulin G decreased, blood immunoglobulin M
decreased, hypogammaglobulinemia, hypoglobulinemia, and immunoglobulins
decreased
8 Hypertransaminasemia includes alanine aminotransferase
increased, aspartate aminotransferase increased, and hepatic enzyme increased
9 Tremor includes essential tremor, intention tremor, and
tremor
10 Encephalopathy includes cognitive disorder, depressed
level of consciousness, disturbance in attention, encephalopathy, lethargy,
leukoencephalopathy, memory impairment, somnolence, and toxic encephalopathy
11 Insomnia includes initial insomnia, insomnia, and terminal
insomnia
12 Rash includes dermatitis contact, eczema, erythema, rash,
and rash maculopapular
|
Additional adverse reactions in patients with MRD-positive
ALL that did not meet the threshold criteria for inclusion in Table 9 were:
Blood and lymphatic system disorders: anemia
General disorders and administration site
conditions: edema peripheral, pain, and chest pain (includes chest pain
and musculoskeletal chest pain)
Hepatobiliary disorders: blood bilirubin increased
Immune system disorders: hypersensitivity and cytokine
release syndrome
Infections and infestations: viral infectious
disorders, bacterial infectious disorders, and fungal infectious disorders
Injury, poisoning and procedural
complications: medication error and overdose (includes overdose and
accidental overdose)
Investigations: blood alkaline phosphatase increased
Musculoskeletal and connective tissue disorders: pain
in extremity and bone pain
Nervous system disorders: seizure (includes seizure
and generalized tonic-clonic seizure), speech disorder, and hypoesthesia
Psychiatric disorders: confusional state,
disorientation, and depression
Respiratory, thoracic and mediastinal
disorders: dyspnea and productive cough
Vascular disorders: hypertension (includes blood
pressure increased and hypertension) flushing (includes flushing and hot
flush), and capillary leak syndrome
PhiladelphiaChromosome-negative Relapsed Or Refractory B-cell
Precursor ALL
The safety data described below reflect exposure to
BLINCYTO in a randomized, open-label, active-controlled clinical study (TOWER
Study) in which 376 patients withPhiladelphiachromosome-negative relapsed or refractory B-cell precursor ALL were treated
with BLINCYTO (n = 267) or standard of care (SOC) chemotherapy (n = 109). The
median age of BLINCYTO-treated patients was 37 years (range: 18 to 80 years),
60% were male, 84% were White, 7% Asian, 2% were Black or African American, 2%
were American Indian or Alaska Native, and 5% were Multiple/Other.
The most common adverse reactions (≥ 20%) in the BLINCYTO
arm were infections (bacterial and pathogen unspecified), pyrexia, headache,
infusion-related reactions, anemia, febrile neutropenia, thrombocytopenia, and
neutropenia. Serious adverse reactions were reported in 62% of patients. The
most common serious adverse reactions (≥ 2%) included febrile neutropenia,
pyrexia, sepsis, pneumonia, overdose, septic shock, CRS, bacterial sepsis,
device related infection, and bacteremia. Adverse reactions of Grade 3 or
higher were reported in 87% of patients. Discontinuation of therapy due to
adverse reactions occurred in 12% of patients treated with BLINCYTO; neurologic
events and infections were the most frequently reported reasons for
discontinuation of treatment due to an adverse reaction. Fatal adverse events
occurred in 16% of patients. The majority of the fatal events were infections.
The adverse reactions occurring at a ≥ 10% incidence for
any grade or ≥ 5% incidence for Grade 3 or higher in the BLINCYTO-treated
patients in first cycle of therapy are summarized in Table 10.
Table 10: Adverse
Reactions Occurring at ≥ 10% Incidence for Any Grade or ≥ 5% Incidence for
Grade 3 or Higher in BLINCYTO-treated Patients in First Cycle of Therapy
|
Adverse Reaction
|
BLINCYTO
(N = 267)
|
Standard of Care (SOC)
Chemotherapy
(N = 109)
|
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
Any Grade*
n (%)
|
≥ Grade 3*
n (%)
|
|
Blood and lymphatic system disorders
|
|
Neutropenia1
|
84 (31)
|
76 (28)
|
67 (61)
|
61 (56)
|
|
Anemia2
|
68 (25)
|
52 (19)
|
45 (41)
|
37 (34)
|
|
Thrombocytopenia3
|
57 (21)
|
47 (18)
|
42 (39)
|
40 (37)
|
|
Leukopenia4
|
21 (8)
|
18 (7)
|
9 (8)
|
9 (8)
|
|
Cardiac disorders
|
|
Arrhythmia5
|
37 (14)
|
5 (2)
|
18 (17)
|
0 (0)
|
|
General disorders and administration site
conditions
|
|
Pyrexia
|
147 (55)
|
15 (6)
|
43 (39)
|
4 (4)
|
|
Edema6
|
48 (18)
|
3 (1)
|
20 (18)
|
1 (1)
|
|
Immune system disorders
|
|
Cytokine release syndrome7
|
37 (14)
|
8 (3)
|
0 (0)
|
0 (0)
|
|
Infections and infestations
|
|
Infections - pathogen unspecified
|
74 (28)
|
40 (15)
|
50 (46)
|
35 (32)
|
|
Bacterial infectious disorders
|
38 (14)
|
19 (7)
|
35 (32)
|
21 (19)
|
|
Viral infectious disorders
|
30 (11)
|
4 (1)
|
14 (13)
|
0 (0)
|
|
Fungal infectious disorders
|
27 (10)
|
13 (5)
|
15 (14)
|
9 (8)
|
|
Injury, poisoning and procedural
complications
|
|
Infusion-related reaction8
|
79 (30)
|
9 (3)
|
9 (8)
|
1 (1)
|
|
Investigations
|
|
Hypertransaminasemia9
|
40 (15)
|
22 (8)
|
13 (12)
|
7 (6)
|
|
Nervous system disorders
|
|
Headache
|
61 (23)
|
1 (<1)
|
30 (28)
|
3 (3)
|
|
Skin and subcutaneous tissue disorders
|
|
Rash10
|
31 (12)
|
2 (1)
|
21 (19)
|
0 (0)
|
|
* Grading based on NCI Common Terminology
Criteria for Adverse Events (CTCAE) version 4.0
1 Neutropenia includes agranulocytosis, febrile neutropenia,
neutropenia, and neutrophil count decreased
2 Anemia includes anemia and hemoglobin decreased
3 Thrombocytopenia includes platelet count decreased and
thrombocytopenia
4 Leukopenia includes leukopenia and white blood cell count
decreased
5 Arrhythmia includes arrhythmia, atrial fibrillation, atrial
flutter, bradycardia, sinus bradycardia, sinus tachycardia, supraventricular
tachycardia, and tachycardia
6 Edema includes face edema, fluid retention, edema, edema
peripheral, peripheral swelling, and swelling face
7 Cytokine release syndrome includes cytokine release syndrome
and cytokine storm
8 Infusion-related reaction is a composite term that includes
the term infusion-related reaction and the following events occurring with
the first 48 hours of infusion and the event lasted ≤ 2 days: pyrexia,
cytokine release syndrome, hypotension, myalgia, acute kidney injury,
hypertension, and rash erythematous
9 Hypertransaminasemia includes alanine aminotransferase
increased, aspartate aminotransferase increased, hepatic enzyme increased,
and transaminases increased
10 Rash includes erythema, rash, rash erythematous, rash generalized,
rash macular, rash maculo-papular, rash pruritic, skin exfoliation, and toxic
skin eruption.
|
Selected laboratory abnormalities worsening from baseline
Grade 0-2 to treatment-related maximal Grade 3-4 in first cycle of therapy are
shown in Table 11.
Table 11: Selected
Laboratory Abnormalities Worsening from Baseline Grade 0-2 to Treatment-related
Maximal Grade 3-4* in First Cycle of Therapy
|
|
BLINCYTO Grade 3 or 4 (%)
|
SOC Chemotherapy Grade 3 or 4
(%)
|
|
Hematology
|
|
Decreased lymphocyte count
|
80
|
83
|
|
Decreased white blood cell count
|
53
|
97
|
|
Decreased hemoglobin
|
29
|
43
|
|
Decreased neutrophil count
|
57
|
68
|
|
Decreased platelet count
|
47
|
85
|
|
Chemistry
|
|
Increased ALT
|
11
|
11
|
|
Increased bilirubin
|
5
|
4
|
|
Increased AST
|
8
|
4
|
|
* Includes only patients who had both baseline
and at least one laboratory measurement during first cycle of therapy
available.
|
Relapsed Or Refractory B-cell
Precursor ALL
Other important adverse reactions from pooled relapsed or
refractory B-cell precursor ALL studies were:
Blood and lymphatic system disorders: lymphadenopathy, hematophagic histiocytosis, and leukocytosis (includes leukocytosis and
white blood cell count increased)
General disorders and administration site
conditions: chills, chest pain (includes chest discomfort, chest pain,
musculoskeletal chest pain, and non-cardiac chest pain), pain, body temperature
increased, hyperthermia, and systemic inflammatory response syndrome
Hepatobiliary disorders: hyperbilirubinemia (includes blood
bilirubin increased and hyperbilirubinemia)
Immune system disorders: hypersensitivity (includes
hypersensitivity, anaphylactic reaction, angioedema, dermatitis allergic, drug eruption, drug
hypersensitivity, erythema multiforme, and urticaria)
Injury, poisoning and procedural
complications: medication error and overdose (includes overdose,
medication error, and accidental overdose)
Investigations: weight increased, decreased
immunoglobulins (includes immunoglobulins decreased, blood immunoglobulin A decreased, blood immunoglobulin G decreased, blood immunoglobulin M decreased, and
hypogammaglobulinemia), blood alkaline phosphatase increased, and
hypertransaminasemia
Metabolism and nutrition disorders: tumor lysis
syndrome
Musculoskeletal and connective tissue disorders: back pain, bone pain, and pain in extremity
Nervous system disorders: tremor (resting tremor,
intention tremor, essential tremor, and tremor), altered state
of consciousness (includes altered state of consciousness, depressed level of
consciousness, disturbance in attention, lethargy, mental status changes, stupor,
and somnolence), dizziness, memory impairment,
seizure (includes seizure, and atonic seizure), aphasia, cognitive disorder, speech disorder, hypoesthesia, encephalopathy,
and cranial nerve disorders (trigeminal neuralgia, trigeminal nerve disorder, sixth
nerve paralysis, cranial nerve disorder, facial nerve disorder, and facial paresis).
Psychiatric disorders: insomnia, disorientation,
confusional state, and depression (includes depressed mood, depression,
suicidal ideation, and completed suicide)
Respiratory, thoracic and mediastinal disorders: dyspnea (includes acute respiratory failure, dyspnea, dyspnea
exertional, respiratory failure, respiratory distress, bronchospasm, bronchial
hyperreactivity, tachypnea, and wheezing), cough, and productive cough
Vascular disorders: hypotension (includes blood pressure
decreased, hypotension, hypovolemic shock, and circulatory collapse), hypertension (includes blood pressure
increased, hypertension, and hypertensive crisis), flushing (includes
flushing and hot flush), and capillary leak syndrome
Postmarketing Experience
The following adverse reactions have been identified during
postapproval use of BLINCYTO. Because these reactions are reported voluntarily
from a population of uncertain size, it is not always possible to reliably
estimate their frequency or establish a causal relationship to drug exposure.
· Fatal pancreatitis has been
reported in patients receiving BLINCYTO in combination with dexamethasone
[see WARNINGS AND PRECAUTIONS].
Immunogenicity
As with all therapeutic proteins, there is potential for
immunogenicity. The immunogenicity of BLINCYTO has been evaluated using either
an electrochemiluminescence detection technology (ECL) or an enzyme-linked immunosorbent assay (ELISA) screening immunoassay for the detection
of binding anti-blinatumomab antibodies. For patients whose sera tested
positive in the screening immunoassay, an in vitro biological assay was
performed to detect neutralizing antibodies.
In clinical studies, less than 2% of patients treated with
BLINCYTO tested positive for binding anti-blinatumomab antibodies. Of patients
who developed anti-blinatumomab antibodies, 7 out of 9 (78%) had in vitro
neutralizing activity. Anti-blinatumomab antibody formation may affect
pharmacokinetics of BLINCYTO.
If formation of anti-blinatumomab antibodies with a
clinically significant effect is suspected, contact Amgen at 1-800-77-AMGEN
(1-800-772-6436) to discuss antibody testing.
The detection of anti-blinatumomab antibody formation is
highly dependent on the sensitivity and specificity of the assay. Additionally,
the observed incidence of antibody (including neutralizing antibody) positivity
in an assay may be influenced by several factors, including assay methodology,
sample handling, timing of sample collection, concomitant medications, and
underlying disease. For these reasons, comparison of the incidence of
antibodies to blinatumomab with the incidence of antibodies to other products
may be misleading.
DRUG INTERACTIONS
No formal drug interaction studies have been conducted with
BLINCYTO. Initiation of BLINCYTO treatment causes transient release of
cytokines that may suppress CYP450 enzymes. The highest drug-drug interaction
risk is during the first 9 days of the first cycle and the first 2 days of the
second cycle in patients who are receiving concomitant CYP450 substrates,
particularly those with a narrow therapeutic index. In these patients, monitor
for toxicity (eg, warfarin) or drug concentrations (eg, cyclosporine). Adjust the dose of the
concomitant drug as needed [see CLINICAL
PHARMACOLOGY].
Warnings
& Precautions
WARNINGS
Included as part of the PRECAUTIONS section.
PRECAUTIONSCytokine Release Syndrome
Cytokine Release Syndrome (CRS), which may be life-threatening
or fatal, occurred in patients receiving BLINCYTO. The median time to onset of
CRS was 2 days after the start of infusion. Manifestations of CRS include
fever, headache, nausea, asthenia, hypotension, increased alanine aminotransferase, increased aspartate aminotransferase, increased total
bilirubin, and disseminated intravascular coagulation (DIC). The manifestations of
CRS after treatment with BLINCYTO overlap with those of infusion reactions,
capillary leak syndrome (CLS), and hemophagocytic histiocytosis/macrophage activation syndrome (MAS).
Using all of these terms to define CRS in clinical trials of BLINCYTO, CRS was
reported in 15% of patients with relapsed or refractory ALL and in 7% of
patients with MRD-positive ALL.
Monitor patients for signs or symptoms of these events.
Advise outpatients on BLINCYTO to contact their healthcare professional for
signs and symptoms associated with CRS. If severe CRS occurs, interrupt
BLINCYTO until CRS resolves. Discontinue BLINCYTO permanently if
life-threatening CRS occurs [see DOSAGE
AND ADMINISTRATION].
Neurological Toxicities
In patients with ALL receiving BLINCYTO in clinical
studies, neurological toxicities have occurred in approximately 65% of
patients. Among patients that experienced a neurologic event, the median time
to the first event was within the first 2 weeks of BLINCYTO treatment and the
majority of events resolved. The most common (≥ 10%) manifestations of
neurological toxicity were headache, and tremor; the neurological toxicity
profile varied by age group [see Use In Specific Populations]. Grade 3 or
higher (severe, life-threatening, or fatal) neurological toxicities following
initiation of BLINCYTO administration occurred in approximately 13% of patients
and included encephalopathy, convulsions, speech disorders, disturbances in
consciousness, confusion and disorientation, and coordination and balance
disorders. Manifestations of neurological toxicity included cranial nerve
disorders. The majority of neurologic events resolved following interruption of
BLINCYTO, but some resulted in treatment discontinuation.
There is limited experience with BLINCYTO in patients with
active ALL in the central nervous system (CNS) or a history
of neurologic events. Patients with a history or presence of clinically relevant
CNS pathology were excluded from clinical
studies.
Monitor patients receiving BLINCYTO for signs and symptoms
of neurological toxicities. Advise outpatients on BLINCYTO to contact their
healthcare professional if they develop signs or symptoms of neurological
toxicities. Interrupt or discontinue BLINCYTO as recommended [see DOSAGE
AND ADMINISTRATION].
Infections
In patients with ALL receiving BLINCYTO in clinical
studies, serious infections such as sepsis, pneumonia, bacteremia, opportunistic infections,
and catheter-site infections were observed in
approximately 25% of patients, some of which were life-threatening or fatal. As
appropriate, administer prophylactic antibiotics and employ
surveillance testing during treatment with BLINCYTO. Monitor patients for signs
and symptoms of infection and treat appropriately.
Tumor Lysis Syndrome
Tumor lysis syndrome (TLS), which may be life-threatening
or fatal, has been observed in patients receiving BLINCYTO. Appropriate
prophylactic measures, including pretreatment nontoxic cytoreduction and
on-treatment hydration, should be used for the prevention of TLS during
BLINCYTO treatment. Monitor for signs or symptoms of TLS. Management of these
events may require either temporary interruption or discontinuation of BLINCYTO
[see DOSAGE AND ADMINISTRATION].
Neutropenia And Febrile
Neutropenia
Neutropenia and febrile neutropenia, including
life-threatening cases, have been observed in patients receiving BLINCYTO.
Monitor laboratory parameters (including, but not limited to, white blood cell count and absolute neutrophil count) during BLINCYTO
infusion. Interrupt BLINCYTO if prolonged neutropenia occurs.
Effects On Ability To Drive And
Use Machines
Due to the potential for neurologic events, including
seizures, patients receiving BLINCYTO are at risk for loss of consciousness
[see Neurological Toxicities]. Advise patients to refrain from driving and
engaging in hazardous occupations or activities such as operating heavy or
potentially dangerous machinery while BLINCYTO is being administered.
Elevated Liver Enzymes
Treatment with BLINCYTO was associated with transient
elevations in liver enzymes. In patients with ALL receiving BLINCYTO in
clinical studies, the median time to onset of elevated liver enzymes was 3
days.
The majority of these transient elevations in liver enzymes
were observed in the setting of CRS. For the events that were observed outside
the setting of CRS, the median time to onset was 19 days. Grade 3 or greater
elevations in liver enzymes occurred in approximately 7% of patients outside
the setting of CRS and resulted in treatment discontinuation in less than 1% of
patients.
Monitor alanine aminotransferase (ALT), aspartate
aminotransferase (AST), gamma-glutamyl transferase (GGT), and total blood
bilirubin prior to the start of and during BLINCYTO treatment. Interrupt
BLINCYTO if the transaminases rise to greater than 5 times the upper limit of
normal or if total bilirubin rises to more than 3 times the upper limit of
normal.
Pancreatitis
Fatal pancreatitis has been reported in patients receiving
BLINCYTO in combination with dexamethasone in clinical studies and the
postmarketing setting [see ADVERSE
REACTIONS].
Evaluate patients who develop signs and symptoms of
pancreatitis. Management of pancreatitis may require either temporary
interruption or discontinuation of BLINCYTO and dexamethasone [see DOSAGE
AND ADMINISTRATION].
Leukoencephalopathy
Cranial magnetic resonance imaging (MRI) changes showing leukoencephalopathy have
been observed in patients receiving BLINCYTO, especially in patients with prior
treatment with cranial irradiation and antileukemic chemotherapy (including systemic
high-dose methotrexate or intrathecal cytarabine).
The clinical significance of these imaging changes is unknown.
Preparation And Administration
Errors
Preparation and administration errors have occurred with
BLINCYTO treatment. Follow instructions for preparation (including admixing)
and administration strictly to minimize medication errors (including underdose
and overdose) [see DOSAGE AND ADMINISTRATION].
Immunization
The safety of immunization with live viral vaccines during or following BLINCYTO
therapy has not been studied. Vaccination with live virus vaccines is
not recommended for at least 2 weeks prior to the start of BLINCYTO treatment,
during treatment, and until immune recovery following last cycle of BLINCYTO.
Risk Of Serious Adverse
Reactions In Pediatric Patients Due To Benzyl Alcohol Preservative
Serious and fatal adverse reactions including “gasping
syndrome” can occur in neonates and infants treated with benzyl
alcohol-preserved drugs, including BLINCYTO (with preservative). The “gasping
syndrome” is characterized by central nervous system depression,
metabolic acidosis, and gasping respirations.
When prescribing BLINCYTO (with preservative) for pediatric
patients, consider the combined daily metabolic load of benzyl alcohol from all
sources including BLINCYTO (with preservative) (contains 7.4 mg of benzyl alcohol per mL) and other drugs
containing benzyl alcohol. The minimum amount of benzyl alcohol at which
serious adverse reactions may occur is not known [see Use In Specific
Populations].
Due to the addition of bacteriostatic saline, 7-day bags of
BLINCYTO solution for infusion with preservative contain benzyl alcohol and are
not recommended for use in any patients weighing less than 22 kg [see DOSAGE
AND ADMINISTRATION and Use In Specific Populations].
Patient Counseling Information
Advise the patient to read the FDA-approved patient
labeling (Medication Guide).
Cytokine Release Syndrome (CRS)
Advise patients of the risk of CRS and infusion reactions,
and to contact their healthcare professional for signs and symptoms associated
with CRS or infusion reactions (pyrexia, fatigue, nausea, vomiting, chills,
hypotension, rash, and wheezing) [see WARNINGS AND
PRECAUTIONS and ADVERSE REACTIONS].
Neurological Toxicities
Advise patients of the risk of neurological toxicities, and
to contact their healthcare professional for signs and symptoms associated with
this event (convulsions, speech disorders, and confusion) [see WARNINGS
AND PRECAUTIONS and ADVERSE
REACTIONS].
Infections
Advise patients of the risk of infections, and to contact
their healthcare professional for signs or symptoms of infection
[see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Inform patients of the importance of keeping the skin clean
around the intravenous catheter to reduce the risk of infection.
Pancreatitis
Advise patients of the risk of pancreatitis and to contact
their healthcare provider for signs or symptoms of pancreatitis, which include
severe and persistent stomach pain, with or without nausea and vomiting
[see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Driving And Engaging In Hazardous
Occupations
Advise patients to refrain from driving and engaging in
hazardous occupations or activities such as operating heavy or potentially
dangerous machinery while BLINCYTO is being administered. Patients should be
advised that they may experience neurological events [see WARNINGS AND
PRECAUTIONS].
Infusion Pump Errors
Inform patients they should not adjust the setting on the
infusion pump. Any changes to pump function may result in dosing errors. If
there is a problem with the infusion pump or the pump alarms, patients should
contact their doctor or nurse immediately.
Nonclinical ToxicologyCarcinogenesis, Mutagenesis,
Impairment Of Fertility
No carcinogenicity or genotoxicity studies have been
conducted with blinatumomab.
No studies have been conducted to evaluate the effects of
blinatumomab on fertility. A murine surrogate molecule had no adverse effects
on male and female reproductive organs in a 13-week repeat-dose toxicity study
in mice.
Use In Specific
PopulationsPregnancyRisk Summary
Based on its mechanism of action, BLINCYTO may cause fetal
harm including B-cell lymphocytopenia when administered to a pregnant woman
[see CLINICAL PHARMACOLOGY]. There are no data on
the use of BLINCYTO in pregnant women. In animal reproduction studies, a murine
surrogate molecule administered to pregnant mice crossed the placental barrier
(see Data). Advise pregnant women of the potential risk to a fetus.
The background rate of major birth defects and miscarriage is unknown for the indicated
population. In theU.S.general population, the estimated background risk of major birth defects and
miscarriage in clinically recognized pregnancies is 2-4% and 15-20%,
respectively.
Clinical Considerations
Fetal/Neonatal Adverse Reactions
Due to the potential for B-cell lymphocytopenia in infants
following exposure to BLINCYTO in-utero, the infant's B lymphocytes should be
monitored before the initiation of live virus vaccination [see WARNINGS
AND PRECAUTIONS].
Data
Animal Data
Animal reproduction studies have not been conducted with
blinatumomab. In embryo-fetal developmental toxicity studies, a murine
surrogate molecule was administered intravenously to pregnant mice during the
period of organogenesis. The surrogate molecule crossed the placental barrier
and did not cause embryo-fetal toxicity or teratogenicity. The expected
depletions of B and T cells were observed in the pregnant mice, but
hematological effects were not assessed in fetuses.
LactationRisk Summary
There is no information regarding the presence of
blinatumomab in human milk, the effects on the breastfed infant, or the effects
on milk production. Because many drugs are excreted in human milk and because
of the potential for serious adverse reactions in nursing infants from
BLINCYTO, including B-cell lymphocytopenia, advise patients not to breastfeed
during and for at least 48 hours after treatment with BLINCYTO.
Females And Males Of
Reproductive Potential
Based on its mechanism of action, BLINCYTO may cause fetal
harm when administered to a pregnant woman [see Use In Specific
Populations].
Pregnancy Testing
Verify the pregnancy status of females of reproductive
potential prior to initiating BLINCYTO treatment.
Contraception
Females
Advise females of reproductive potential to use effective
contraception during treatment and for at least 48 hours after the last dose of
BLINCYTO.
Pediatric Use
The safety and efficacy of BLINCYTO have been established
in pediatric patients with relapsed or refractory B-cell precursor ALL. Use of
BLINCYTO is supported by a single-arm trial in pediatric patients with relapsed
or refractory B-cell precursor ALL. This study included pediatric patients in
the following age groups: 10 infants (1 month up to less than 2 years), 40
children (2 years up to less than 12 years), and 20 adolescents (12 years to
less than 18 years). No differences in efficacy were observed between the
different age subgroups. The efficacy has also been established based on
extrapolation from adequate and well-controlled studies in adults with
MRD-positive B-cell precursor ALL.
In general, the adverse reactions in BLINCYTO-treated
pediatric patients were similar in type to those seen in adult patients with
relapsed or refractory B-cell precursor ALL [see ADVERSE
REACTIONS]. Adverse reactions that were observed more frequently (≥
10% difference) in the pediatric population compared to the adult population
were pyrexia (80% vs. 61%), hypertension (26% vs. 8%), anemia (41% vs. 24%), infusion-related
reaction (49% vs. 34%), thrombocytopenia (34% vs. 21%), leukopenia (24% vs. 11%), and weight
increased (17% vs. 6%).
In pediatric patients less than 2 years old (infants), the
incidence of neurologic toxicities was not significantly different than for the
other age groups, but its manifestations were different; the only event terms
reported were agitation, headache, insomnia, somnolence, and irritability.
Infants also had an increased incidence of hypokalemia (50%) compared to other pediatric
age cohorts (15-20%) or adults (17%).
The steady-state concentrations of blinatumomab were
comparable in adult and pediatric patients at the equivalent dose levels based
on BSA-based regimens.
Benzyl Alcohol Toxicity In
Pediatric Patients
Serious adverse reactions including fatal reactions and the
“gasping syndrome” occurred in premature neonates and infants in the neonatal intensive care unit who received
drugs containing benzyl alcohol as a preservative. In these cases, benzyl
alcohol dosages of 99 to 234 mg/kg/day produced high levels of benzyl alcohol
and its metabolites in the blood and urine (blood levels of benzyl alcohol were
0.61 to 1.378 mmol/L). Additional adverse reactions included gradual
neurological deterioration, seizures, intracranial hemorrhage, hematologic
abnormalities, skin breakdown, hepatic and renal failure, hypotension, bradycardia, and cardiovascular collapse. Preterm,
low-birth weight infants may be more likely to develop these reactions because
they may be less able to metabolize benzyl alcohol.
When prescribing BLINCYTO (with preservative) in pediatric
patients, consider the combined daily metabolic load of benzyl alcohol from all
sources including BLINCYTO (with preservative) (contains 7.4 mg of benzyl
alcohol per mL) and other drugs containing benzyl alcohol. The minimum amount
of benzyl alcohol at which serious adverse reactions may occur is not known
[see WARNINGS AND PRECAUTIONS].
Due to the addition of bacteriostatic saline, 7-day bags of
BLINCYTO solution for infusion contain benzyl alcohol and are not recommended
for use in patients weighing less than 22 kg. Prepare BLINCYTO solution for
infusion with preservative-free saline (24- or 48-hour bags) for use in
patients weighing less than 22 kg [see DOSAGE
AND ADMINISTRATION].
Geriatric Use
Of the total number of patients with ALL treated in
clinical studies of BLINCYTO approximately 12% were 65 and over, while 2% were
75 and older. No overall differences in safety or effectiveness were observed
between these patients and younger patients, and other reported clinical
experience has not identified differences in responses between the elderly and
younger patients. However, elderly patients experienced a higher rate of
serious infections and neurological toxicities, including cognitive disorder,
encephalopathy, and confusion [see WARNINGS AND PRECAUTIONS].
Overdosage
& Contraindications
OVERDOSE
Overdoses have been observed, including one adult patient
who received 133-fold the recommended therapeutic dose of BLINCYTO delivered
over a short duration.
In the dose evaluation phase of the Phase ½ study in
pediatric and adolescent patients with relapsed or refractory B-cell precursor
ALL, one patient experienced a fatal cardiac failure event in the setting of
life-threatening cytokine release syndrome (CRS) at a 30 mcg/m²/day (higher
than the maximum tolerated/recommended) dose [see WARNINGS AND PRECAUTIONS and ADVERSE
REACTIONS].
Overdoses resulted in adverse reactions, which were
consistent with the reactions observed at the recommended therapeutic dose and
included fever, tremors, and headache. In the event of overdose, interrupt the
infusion, monitor the patient for signs of toxicity, and provide supportive care [see WARNINGS
AND PRECAUTIONS]. Consider re-initiation of
BLINCYTO at the correct therapeutic dose when all toxicities have resolved and
no earlier than 12 hours after interruption of the infusion [see DOSAGE
AND ADMINISTRATION].
CONTRAINDICATIONS
BLINCYTO is contraindicated in patients with known
hypersensitivity to blinatumomab or to any component of the product
formulation.
Clinical
Pharmacology
CLINICAL PHARMACOLOGYMechanism Of Action
Blinatumomab is a bispecific CD19-directed CD3 T-cell
engager that binds to CD19 expressed on the surface of cells of B-lineage
origin and CD3 expressed on the surface of T cells. It activates endogenous T cells by connecting CD3 in
the T-cell receptor (TCR) complex with CD19
on benign and malignant B cells. Blinatumomab mediates
the formation of a synapse between the T-cell and the tumor
cell, upregulation of cell adhesion molecules,
production of cytolytic proteins, release of inflammatory cytokines, and
proliferation of T cells, which result in redirected lysis of CD19+ cells.
Pharmacodynamics
During the continuous intravenous infusion over 4 weeks,
the pharmacodynamic response was characterized by T-cell activation and initial
redistribution, reduction in peripheral B cells, and transient cytokine
elevation.
Peripheral T-cell redistribution (ie, T-cell adhesion to
blood vessel endothelium and/or transmigration into
tissue) occurred after start of BLINCYTO infusion or dose escalation. T-cell
counts initially declined within 1 to 2 days and then returned to baseline
levels within 7 to 14 days in the majority of patients. Increase of T-cell
counts above baseline (T-cell expansion) was observed in few patients.
Peripheral B cell counts decreased to less than or
equal to 10 cells/microliter during the first treatment cycle at doses ≥ 5
mcg/m²/day or ≥ 9 mcg/day in the majority of patients. No recovery of
peripheral B-cell counts was observed during the 2-week BLINCYTO-free period between
treatment cycles. Incomplete depletion of B cells occurred at doses of 0.5
mcg/m²/day and 1.5 mcg/m²/day and in a few patients at higher doses.
Cytokines including IL-2, IL-4, IL-6, IL-8, IL-10, IL-12, TNF-α, and IFN-γ were measured, and IL-6,
IL-10, and IFN-γ were elevated. The highest elevation of cytokines was observed
in the first 2 days following start of BLINCYTO infusion. The elevated cytokine
levels returned to baseline within 24 to 48 hours during the infusion. In
subsequent treatment cycles, cytokine elevation occurred in fewer patients with
lesser intensity compared to the initial 48 hours of the first treatment cycle.
Pharmacokinetics
The pharmacokinetics of blinatumomab appear linear over a dose
range from 5 to 90 mcg/m²/day (approximately equivalent to 9 to 162 mcg/day) in
adult patients. Following continuous intravenous infusion, the steady-state
serum concentration (Css) was achieved within a day and remained stable over
time. The increase in mean Css values was approximately proportional to the
dose in the range tested. At the clinical doses of 9 mcg/day and 28 mcg/day for
the treatment of relapsed or refractory ALL, the mean (SD) Css was 228 (356)
pg/mL and 616 (537) pg/mL, respectively.
Distribution
The estimated mean (SD) volume of distribution based on
terminal phase (Vz) was 4.35 (2.45) L with continuous intravenous infusion of
blinatumomab.
Metabolism
The metabolic pathway of blinatumomab has not been
characterized. Like other protein therapeutics, BLINCYTO is expected to be
degraded into small peptides and amino acids via catabolic pathways.
Elimination
The estimated mean (SD) systemic clearance with continuous
intravenous infusion in patients receiving blinatumomab in clinical studies was
3.11 (2.98) L/hour. The mean (SD) half-life was 2.10 (1.41) hours. Negligible
amounts of blinatumomab were excreted in the urine at the tested clinical
doses.
Gender, Age, And Body Surface
Area
Results of population pharmacokinetic analyses indicate
that age (0.62 to 80 years of age) and gender do not influence the
pharmacokinetics of blinatumomab. Body surface area (0.4 to 2.70 m²) influences
the pharmacokinetics of blinatumomab, however, the clinical relevance of this
effect is unknown.
Hepatic Impairment
No formal pharmacokinetic studies using BLINCYTO have been
conducted in patients with hepatic impairment.
Renal Impairment
No formal pharmacokinetic studies of blinatumomab have been
conducted in patients with renal impairment.
Pharmacokinetic analyses showed an approximately 2-fold
difference in mean blinatumomab clearance values between patients with moderate
renal impairment (CrCL ranging from 30 to 59 mL/min, N = 21) and normal renal
function (CrCL more than 90 mL/min, N = 215). However, high interpatient
variability was discerned (CV% up to 96.8%), and clearance values in renal
impaired patients were essentially within the range observed in patients with
normal renal function. There is no information available in patients with
severe renal impairment (CrCL less than 30 mL/min) or patients on hemodialysis.
Drug Interactions
Transient elevation of cytokines may suppress CYP450 enzyme
activities [see DRUG INTERACTIONS and Pharmacodynamics].
Specific PopulationsPediatrics
The pharmacokinetics of blinatumomab appear linear over a
dose range from 5 to 30 mcg/m²/day in pediatric patients. At the recommended
doses, the mean (SD) steady-state concentration (Css) values were 162 (179) and
533 (392) pg/mL at 5 and 15 mcg/m²/day doses, respectively. The estimated mean
(SD) volume of distribution (Vz), clearance (CL), and terminal half-life (t½,z)
were 3.14 (2.97) L/m², 1.88 (1.90) L/hour/m², and 2.04 (1.35) hours,
respectively.
Clinical StudiesMRD-positive B-cell Precursor
ALLBLAST Study
The efficacy of BLINCYTO was evaluated in an open-label, multicenter,
single-arm study (BLAST Study) [NCT01207388] that included
patients who were ≥ 18 years of age, had received at least 3 chemotherapy
blocks of standard ALL therapy, were in hematologic complete remission (defined
as < 5% blasts in bone marrow, absolute neutrophil count > 1 Gi/L, platelets
> 100 Gi/L) and had MRD at a level of ≥ 0.1% using an assay with a minimum
sensitivity of 0.01%. BLINCYTO was administered at a constant dose of 15
mcg/m²/day (equivalent to the recommended dosage of 28 mcg/day) intravenously
for all treatment cycles. Patients received up to 4 cycles of treatment. Dose
adjustment was possible in case of adverse events.
The treated population included 86 patients in first or
second hematologic complete remission (CR1 or CR2). The demographics and baseline
characteristics are shown in Table 12. The median number of treatment cycles
was 2 (range: 1 to 4). Following treatment with BLINCYTO, 45 out of 61 (73.8%)
patients in CR1 and 14 out of 25 (56.0%) patients in CR2 underwent allogeneic hematopoietic stem cell transplantation in continuous
hematologic complete remission.
Table 12:
Demographics and Baseline Characteristics in BLAST Study
|
Characteristic
|
BLINCYTO
(N = 86)
|
|
Age
|
|
Median, years (min, max)
|
43 (18,76)
|
|
≥ 65 years, n (%)
|
10 (12)
|
|
Males, n (%)
|
50 (58)
|
|
Race, n (%)
|
|
Asian
|
1 (1)
|
|
Other (mixed)
|
0 (0)
|
|
White
|
76 (88)
|
|
Unknown
|
9 (11)
|
|
Philadelphia chromosome disease status, n (%)
|
|
Positive
|
1 (1)
|
|
Negative
|
85 (99)
|
|
Relapse history, n (%)
|
|
Patients in 1st CR
|
61 (71)
|
|
Patients in 2nd CR
|
25 (29)
|
|
MRD level at baseline*, n (%)
|
|
≥ 10%
|
7 (8)
|
|
≥ 1% and < 10%
|
34 (40)
|
|
≥ 0.1% and < 1%
|
45 (52)
|
|
* Assessed centrally using an assay with
minimum sensitivity of 0.01%
|
Efficacy was based on achievement of undetectable MRD
within one cycle of BLINCYTO treatment and hematological relapse-free survival
(RFS). The assay used to assess MRD response had a sensitivity of 0.01% for 6
patients and < 0.005% for 80 patients. Overall, undetectable MRD was
achieved by 70 patients (81.4%: 95% CI: 71.6%, 89.0%). The median hematological
RFS was 22.3 months. Table 13 shows the MRD response and hematological RFS by
remission number.
Table 13: Efficacy
Results in Patients ≥ 18 Years of Age With MRD-positive B-cell Precursor ALL
(BLAST Study)
|
|
Patients in CR1
(n=61)
|
Patients in CR2
(n=25)
|
|
Complete MRD response1, n (%),
[95% CI]
|
52 (85.2)
[73.8, 93.0]
|
18 (72.0)
[50.6, 87.9]
|
|
Median hematological relapse-free survival2 in
months (range)
|
35.2 (0.4, 53.5)
|
12.3 (0.7, 42.3)
|
|
1 Complete MRD response was defined as the
absence of detectable MRD confirmed in an assay with minimum sensitivity of
0.01%
2 Relapse was defined as either hematological or
extramedullary relapse, secondary leukemia, or death due to any cause;
Includes time after transplantation; Kaplan Meier estimate
|
Undetectable MRD was achieved by 65 of 80 patients (81.3%:
95% CI: 71.0%, 89.1%) with an assay sensitivity of at least 0.005%. The
estimated median hematological RFS among the 80 patients using the higher
sensitivity assay was 24.2 months (95% CI: 17.9, NE).
Relapsed/Refractory B-cell
Precursor ALLTOWER Study
The efficacy of BLINCYTO was compared to standard of care
(SOC) chemotherapy in a randomized, open-label, multicenter study (TOWER Study)
[NCT02013167]. Eligible patients were ≥ 18 years of age with relapsed or
refractory B-cell precursor ALL [> 5% blasts in the bone marrow and
refractory to primary induction therapy or refractory to last therapy,
untreated first relapse with first remission duration < 12 months, untreated
second or later relapse, or relapse at any time after allogeneic hematopoietic
stem cell transplantation (alloHSCT)]. BLINCYTO was administered at 9 mcg/day
on Days 1-7 and 28 mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days
1-28 for Cycles 2-5 in 42-day cycles and for Cycles 6-9 in 84-day cycles. Dose
adjustment was possible in case of adverse events. SOC chemotherapy included
fludarabine, cytarabine arabinoside, and granulocyte colony-stimulating factor
(FLAG); high-dose cytarabine arabinoside (HiDAC); high-dose methotrexate-
(HDMTX) based combination; or clofarabine/clofarabine-based regimens.
There were 405 patients randomized 2:1 to receive BLINCYTO
or investigator-selected SOC chemotherapy. Randomization was stratified by age
(< 35 years vs. ≥ 35 years of age), prior salvage therapy (yes vs. no), and
prior alloHSCT (yes vs. no) as assessed at the time of consent. The
demographics and baseline characteristics were well-balanced between the two
arms (see Table 14).
Table 14:
Demographics and Baseline Characteristics in TOWER Study
|
Characteristic
|
BLINCYTO
(N = 271)
|
Standard of Care (SOC)
Chemotherapy
(N = 134)
|
|
Age
|
|
Median, years (min, max)
|
37 (18, 80)
|
37 (18, 78)
|
|
< 35 years, n (%)
|
124 (46)
|
60 (45)
|
|
≥ 35 years, n (%)
|
147 (54)
|
74 (55)
|
|
≥ 65 years, n (%)
|
33 (12)
|
15 (11)
|
|
≥ 75 years, n (%)
|
10 (4)
|
2 (2)
|
|
Males, n (%)
|
162 (60)
|
77 (58)
|
|
Race, n (%)
|
|
American Indian orAlaskaNative
|
4 (2)
|
1 (1)
|
|
Asian
|
19 (7)
|
9 (7)
|
|
Black (or African American)
|
5 (2)
|
3 (2)
|
|
Multiple
|
2 (1)
|
0
|
|
Native Hawaiian or Other Pacific Islander
|
1 (0)
|
1 (1)
|
|
Other
|
12 (4)
|
8 (6)
|
|
White
|
228 (84)
|
112 (84)
|
|
Prior salvage therapy
|
171 (63)
|
70 (52)
|
|
Prior alloHSCT1
|
94 (35)
|
46 (34)
|
|
Eastern Cooperative Group Status - n (%)
|
|
0
|
96 (35)
|
52 (39)
|
|
1
|
134 (49)
|
61 (46)
|
|
2
|
41 (15)
|
20 (15)
|
|
Unknown
|
0
|
1 (1)
|
|
Refractory to salvage treatment - n (%)
|
|
Yes
|
87 (32)
|
34 (25)
|
|
No
|
182 (67)
|
99 (74)
|
|
Unknown
|
2 (1)
|
1 (1)
|
|
Maximum of central/local bone marrow
blasts - n (%)
|
|
≤ 5%
|
0
|
0
|
|
> 5 to < 10%
|
9 (3)
|
7 (5)
|
|
10 to < 50%
|
60 (22)
|
23 (17)
|
|
≥ 50%
|
201 (74)
|
104 (78)
|
|
Unknown
|
1 (0)
|
0
|
|
1 alloHSCT = allogeneic hematopoietic stem cell
transplantation
|
Of the 271 patients randomized to the BLINCYTO arm, 267
patients received BLINCYTO treatment. The median number of treatment cycles was
two (range: 1 to 9 cycles); 267 (99%) received Cycles 1-2 (induction), 86 (32%)
received Cycles 3-5 (consolidation), and 27 (10%) received Cycles 6-9
(continued therapy). Of the 134 patients on the SOC arm, 25 dropped out prior
to start of study treatment, and 109 patients received a median of 1 treatment
cycle (range: 1 to 4 cycles).
The determination of efficacy was based on overall survival
(OS). The study demonstrated statistically
significant improvement in OS for patients treated with BLINCYTO as compared to
SOC chemotherapy. See Figure 1 and Table 15 below for efficacy results from the
TOWER Study.
Figure 1:
Kaplan-Meier Curve of Overall Survival in TOWER Study
Table 15: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Negative
Relapsed or Refractory B-cell Precursor ALL (TOWER Study)
|
|
BLINCYTO
(N = 271)
|
SOC Chemotherapy
(N = 134)
|
|
Overall Survival
|
|
Number of deaths (%)
|
164 (61)
|
87 (65)
|
|
Median, months [95% CI]
|
7.7 [5.6, 9.6]
|
4.0 [2.9, 5.3]
|
|
Hazard Ratio [95% CI]1
|
0.71 [0.55, 0.93]
|
|
p-value2
|
0.012
|
|
Overall Response
|
|
CR4/CRh*5, n (%)
[95% CI]
|
115 (42) [37, 49]
|
27 (20) [14, 28]
|
|
Treatment difference [95% CI]
|
22 [13, 31]
|
|
p-value3
|
< 0.001
|
|
CR, n (%) [95% CI]
|
91 (34) [28, 40]
|
21 (16) [10, 23]
|
|
Treatment difference [95% CI]
|
18 [10, 26]
|
|
p-value3
|
< 0.001
|
|
MRD Response6 for CR/CRh*
|
|
n1/n2 (%)7 [95% CI]
|
73/115 (64) [54, 72]
|
14/27 (52) [32, 71]
|
|
1 Based on stratified Cox’s model.
2 The p-value was derived using stratified log rank test.
3 The p-value was derived using Cochran-Mantel-Haenszel test.
4 CR (complete remission) was defined as ≤ 5% blasts in the
bone marrow, no evidence of disease, and full recovery of peripheral blood
counts (platelets > 100,000/microliter and absolute neutrophil counts
[ANC] > 1,000/microliter).
5 CRh* (complete remission with partial hematologic recovery)
was defined as ≤ 5% blasts in the bone marrow, no evidence of disease, and
partial recovery of peripheral blood counts (platelets > 50,000/microliter
and ANC > 500/microliter).
6 MRD (minimum residual disease) response was defined as MRD
by PCR or flow cytometry < 1 x 10-4 (0.01%).
7 n1: number of patients who achieved MRD response and
CR/CRh*; n2: number of patients who achieved CR/CRh* and had a postbaseline
assessment.
|
Study MT103-211
Study MT103-211 [NCT01466179] was an open-label,
multicenter, single-arm study. Eligible patients were ≥ 18 years of age with
Philadelphia chromosome-negative relapsed or refractory B-cell precursor ALL
(relapsed with first remission duration of ≤ 12 months in first salvage or
relapsed or refractory after first salvage therapy or relapsed within 12 months
of alloHSCT, and had ≥ 10% blasts in bone marrow).
BLINCYTO was administered as a continuous intravenous
infusion. The recommended dose for this study was determined to be 9 mcg/day on
Days 1-7 and 28 mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days 1-28
for subsequent cycles. Dose adjustment was possible in case of adverse events.
The treated population included 185 patients who received at least 1 infusion
of BLINCYTO; the median number of treatment cycles was 2 (range: 1 to 5).
Patients who responded to BLINCYTO but later relapsed had the option to be
retreated with BLINCYTO. Among treated patients, the median age was 39 years
(range: 18 to 79 years), 63 out of 185 (34.1%) had undergone HSCT prior to
receiving BLINCYTO, and 32 out of 185 (17.3%) had received more than 2 prior
salvage therapies.
Efficacy was based on the complete remission (CR) rate,
duration of CR, and proportion of patients with an MRD-negative CR/CR with
partial hematological recovery (CR/CRh*) within 2 cycles of treatment with
BLINCYTO. Table 16 shows the efficacy results from this study. The HSCT rate
among those who achieved CR/CRh* was 39% (30 out of 77).
Table 16: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Negative
Relapsed or Refractory B-cell Precursor ALL (Study MT103-211)
|
|
N = 185
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
60 (32.4) [25.7 - 39.7]
|
17 (9.2) [5.4 - 14.3]
|
77 (41.6) [34.4 - 49.1]
|
|
MRD response3
|
|
n1/n2 (%)4
|
48/60 (80.0)
|
10/17 (58.8)
|
58/77 (75.3)
|
|
[95% CI]
|
[67.7 - 89.2]
|
[32.9 - 81.6]
|
[64.2 - 84.4]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.7 (0.46 - 16.5)
|
5.0 (0.13 - 8.8)
|
5.9 (0.13 - 16.5)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of disease, and full recovery of
peripheral blood counts (platelets > 100,000/microliter and absolute
neutrophil counts [ANC] > 1,000/microliter).
2 CRh* (complete remission with partial hematological
recovery) was defined as ≤ 5% of blasts in the bone marrow, no evidence of
disease, and partial recovery of peripheral blood counts (platelets >
50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. Six CR/CRh* responders with missing MRD data
were considered as MRD-nonresponders.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
|
ALCANTARA Study
The efficacy of BLINCYTO for treatment ofPhiladelphiachromosome-positive B-cell
precursor ALL was evaluated in an open-label, multicenter, single-arm study
(ALCANTARA Study) [NCT02000427]. Eligible patients were ≥ 18 years of age withPhiladelphiachromosome-positive B-cell precursor ALL, relapsed or refractory to at least 1
second generation or later tyrosine kinase inhibitor (TKI), or intolerant to
second generation TKI, and intolerant or refractory to imatinib mesylate.
BLINCYTO was administered at 9 mcg/day on Days 1-7 and 28
mcg/day on Days 8-28 for Cycle 1, and 28 mcg/day on Days 1-28 for subsequent
cycles. Dose adjustment was possible in case of adverse events.
The treated population included 45 patients who received at
least one infusion of BLINCYTO; the median number of treatment cycles was 2
(range: 1 to 5). The demographics and baseline characteristics are shown in
Table 17.
Table 17:
Demographics and Baseline Characteristics in ALCANTARA Study
|
Characteristic
|
BLINCYTO
(N = 45)
|
|
Age
|
|
Median, years (min, max)
|
55 (23, 78)
|
|
≥ 65 years and < 75 years, n (%)
|
10 (22)
|
|
≥ 75 years, n (%)
|
2 (4)
|
|
Males, n (%)
|
24 (53)
|
|
Race, n (%)
|
|
Asian
|
1 (2)
|
|
Black (or African American)
|
3 (7)
|
|
Other
|
2 (4)
|
|
White
|
39 (87)
|
|
Disease History
|
|
Prior TKI treatment1, n (%)
|
|
1
|
7 (16)
|
|
2
|
21 (47)
|
|
≥ 3
|
17 (38)
|
|
Prior salvage therapy
|
31 (62)
|
|
Prior alloHSCT2
|
20(44)
|
|
Bone marrow blasts3
|
|
≥ 50% to < 75%
|
6 (13)
|
|
≥ 75%
|
28(62)
|
|
1 Number of patients that failed ponatinib = 23
(51%)
2 alloHSCT = allogeneic hematopoietic stem cell
transplantation
3 centrally assessed
|
Efficacy was based on the complete remission (CR) rate,
duration of CR, and proportion of patients with an MRD-negative CR/CR with
partial hematological recovery (CR/CRh*) within 2 cycles of treatment with
BLINCYTO. Table 18 shows the efficacy results from ALCANTARA Study. Five of the
16 responding (31%) patients underwent allogeneic HSCT in CR/CRh* induced with
BLINCYTO. There were 10 patients with document T315I mutation; four
achieved CR within 2 cycles of treatment with BLINCYTO.
Table 18: Efficacy
Results in Patients ≥ 18 Years of Age With Philadelphia Chromosome-Positive
Relapsed or Refractory B-cell Precursor ALL (ALCANTARA Study)
|
|
N = 45
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
14 (31) [18 - 47]
|
2 (4) [1 - 15]
|
16 (36) [22 - 51]
|
|
MRD response3
|
|
n1/n2 (%)4
|
12/14 (86)
|
2/2 (100)
|
14/16 (88)
|
|
[95% CI]
|
[57 - 98]
|
[16, 100]
|
[62 - 98]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.7 (3.6 - 12.0)
|
NE6 (3.7 - 9.0)
|
6.7 (3.6 - 12.0)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of disease, and full recovery of
peripheral blood counts (platelets > 100,000/microliter and absolute
neutrophil counts [ANC] > 1,000/microliter).
2 CRh* (complete remission with partial hematological
recovery) was defined as ≤ 5% of blasts in the bone marrow, no evidence of
disease, and partial recovery of peripheral blood counts (platelets >
50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. Six CR/CRh* responders with missing MRD data were
considered as MRD-nonresponders.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
6 NE = not estimable
|
Study MT103-205
Study MT103-205 [NCT01471782] was an open-label,
multicenter, single-arm study in pediatric patients with relapsed or refractory
B-cell precursor ALL (second or later bone marrow relapse, any marrow relapse
after allogeneic HSCT, or refractory to other treatments, and had > 25%
blasts in bone marrow). BLINCYTO was administered at 5 mcg/m²/day on Days 1-7
and 15 mcg/m²/day on Days 8-28 for Cycle 1, and 15 mcg/m²/day on Days 1-28 for
subsequent cycles. Dose adjustment was possible in case of adverse events.
Patients who responded to BLINCYTO but later relapsed had the option to be
retreated with BLINCYTO.
Among the 70 treated patients, the median age was 8 years
(range: 7 months to 17 years), 40 out of 70 (57.1%) had undergone allogeneic
HSCT prior to receiving BLINCYTO, and 39 out of 70 (55.7%) had refractory
disease. The median number of treatment cycles was 1 (range: 1 to 5).
Twenty-three out of 70 (32.9%) patients achieved CR/CRh*
within the first 2 treatment cycles with 17 out of 23 (73.9%) occurring within
Cycle 1 of treatment. See Table 19 for the efficacy results from the study. The
HSCT rate among those who achieved CR/CRh* was 48% (11 out of 23).
Table 19: Efficacy
Results in Patients < 18 Years of Age With Relapsed or Refractory B-cell
Precursor ALL (Study MT103-205)
|
|
N = 70
|
|
CR1
|
CRh*2
|
CR/CRh*
|
|
n (%) [95% CI]
|
12 (17.1)
[9.2 - 28.0]
|
11 (15.7)
[8.1 - 26.4]
|
23 (32.9)
[22.1 - 45.1]
|
|
MRD response3
|
|
n1/n2 (%)4[95% CI]
|
6/12 (50.0)
[21.1 - 78.9]
|
4/11 (36.4)
[10.9 - 69.2]
|
10/23 (43.5)
[23.2 - 65.5]
|
|
DOR/RFS5
|
|
Median (months) (range)
|
6.0 (0.5 - 12.1)
|
3.5 (0.5 - 16.4)
|
6.0 (0.5 - 16.4)
|
|
1 CR (complete remission) was defined as ≤ 5% of
blasts in the bone marrow, no evidence of circulating blasts or
extra-medullary disease, and full recovery of peripheral blood counts
(platelets > 100,000/microliter and absolute neutrophil counts [ANC] >
1,000/microliter).
2 CRh* (complete remission with partial hematological recovery)
was defined as ≤ 5% of blasts in the bone marrow, no evidence of circulating
blasts or extra-medullary disease, and partial recovery of peripheral blood
counts (platelets > 50,000/microliter and ANC > 500/microliter).
3 MRD (minimal residual disease) response was defined as MRD
by PCR or flow cytometry < 1 x 10-4 (0.01%).
4 n1: number of patients who achieved MRD response and the
respective remission status; n2: number of patients who achieved the
respective remission status. One CR/CRh* responder with missing MRD data was
considered as a MRD-nonresponder.
5 DOR (duration of response)/RFS (relapse-free survival) was
defined as time since first response of CR or CRh* to relapse or death,
whichever is earlier. Relapse was defined as hematological relapse (blasts in
bone marrow greater than 5% following CR) or an extramedullary relapse.
|
Medication
Guide
PATIENT INFORMATION
BLINCYTO®
(blin sye' toe)
(blinatumomab) for injection
What is the most important information I should know about
BLINCYTO?
Call your healthcare provider or get emergency medical help
right away if you get any of the symptoms listed below.
BLINCYTO may cause serious side effects that can be severe,
life-threatening, or lead to death, including:
· Cytokine Release Syndrome (CRS)
and Infusion Reactions. Symptoms of CRS and infusion reactions may
include:
o fever
o tiredness or weakness
o dizziness
o headache
o low blood pressure
o nausea
o vomiting
o chills
o face swelling
o wheezing or trouble breathing
o skin rash
· Neurologic
problems. Symptoms of neurologic problems may include:
o seizures
o difficulty in speaking or slurred speech
o loss of consciousness
o trouble sleeping
o confusion and disorientation
o loss of balance
o headache
o difficulty with facial movements, hearing, vision, or swallowing
Your healthcare provider will check for these problems
during treatment with BLINCYTO. Your healthcare provider may temporarily stop
or completely stop your treatment with BLINCYTO, if you have severe side
effects.
See “What are the possible side effects of
BLINCYTO?” below for other side effects of BLINCYTO.
What is BLINCYTO?
BLINCYTO is a prescription medicine used to treat adults
and children with:
· B-cell precursor acute
lymphoblastic leukemia (ALL) in remission with molecular evidence of leukemia
· B-cell precursor ALL that has
come back or did not respond to previous treatments
ALL is a cancer of the blood in which a particular kind of
white blood cell is growing out of control.
Who should not receive BLINCYTO?
Do not receive BLINCYTO if you are allergic to blinatumomab
or to any of the ingredients of BLINCYTO. See the end of this Medication Guide
for a complete list of ingredients in BLINCYTO.
Before receiving BLINCYTO, tell your healthcare provider
about all of your medical conditions, including if you or your child:
· have a history of neurological
problems, such as seizures, confusion, trouble speaking or loss of balance
· have an infection
· have ever had an infusion
reaction after receiving BLINCYTO or other medications
· have a history of radiation treatment to the brain, or
chemotherapy treatment
· are scheduled to receive a
vaccine. You should not receive a “live vaccine” within 2 weeks before you
start treatment with BLINCYTO, during treatment, and until your immune system recovers after you receive
your last cycle of BLINCYTO. If you are not sure about the type of vaccine, ask
your healthcare provider.
· are pregnant or plan to become
pregnant. BLINCYTO may harm your unborn baby. Tell your healthcare provider if
you become pregnant during treatment with BLINCYTO.
o If you are able to become pregnant, your healthcare provider should
do a pregnancy test before you start treatment with BLINCYTO.
o Females who are able to become pregnant should use an effective form
of birth control during treatment with BLINCYTO, and for at least 48 hours
after the last dose of BLINCYTO.
· are breastfeeding or plan to
breastfeed. It is not known if BLINCYTO passes into your breast milk. You
should not breastfeed during treatment with BLINCYTO and for at least 48 hours
after your last treatment.
Tell your healthcare provider about all the medicines you
take, including prescription and over-the-counter medicines, vitamins, and
herbal supplements.
How will I receive BLINCYTO?
· BLINCYTO will be given to you
by intravenous (IV) infusion into your vein by an infusion pump.
· Your healthcare provider will
decide the number of treatment cycles of BLINCYTO.
o You will receive BLINCYTO by continuous IV infusion for 4 weeks (28
days), followed by a 2 week (14 days) break during which you will not receive
BLINCYTO. This is 1 treatment cycle (42 days).
· Your healthcare provider may
prescribe continued therapy.
o You will receive BLINCYTO by continuous IV infusion for 4 weeks (28
days), followed by an 8 week (56 days) break during which you will not receive
BLINCYTO. This is 1 treatment cycle (84 days).
· Your healthcare provider may
give you BLINCYTO in a hospital or clinic for the first 3 to 9 days of the
first treatment cycle and for the first 2 days of the second cycle to check you
for side effects. If you receive additional treatment cycles of BLINCYTO or if
your treatment is stopped for a period of time and restarted, you may also be
treated in a hospital or clinic.
· Your healthcare provider may
change your dose of BLINCYTO, delay, or completely stop treatment with BLINCYTO
if you have certain side effects.
· Your healthcare provider will
do blood tests during treatment with BLINCYTO to check you for side effects.
· Before you receive BLINCYTO,
you will be given a corticosteroid medicine to help reduce infusion
reactions.
· It is very important to keep
the area around the IV catheter clean to reduce the risk of getting an
infection. Your healthcare provider will show you how to care for your catheter
site.
· Do not change the settings on
your infusion pump, even if there is a problem with your pump or your pump
alarm sounds. Any changes to your infusion pump settings may cause a dose that
is too high or too low to be given.
Call your healthcare provider or nurse right away if you
have any problems with your pump or your pump alarm sounds.
What should I avoid while receiving BLINCYTO?
Do not drive, operate heavy machinery, or do other
dangerous activities while you are receiving BLINCYTO because BLINCYTO can
cause neurological symptoms, such as dizziness, seizures, and confusion.
What are the possible side effects of BLINCYTO?
BLINCYTO may cause serious side effects, including:
See “What is the most important information I should
know about BLINCYTO?”
· Infections. BLINCYTO may
cause life-threatening infections that may lead to death. Tell your healthcare
provider right away if you develop any signs or symptoms of an infection.
· Low white blood cell counts
(neutropenia). Neutropenia is common with BLINCYTO treatment and may
sometimes be life-threatening. Low white blood cell counts can increase your
risk of infection. Your healthcare provider will do blood tests to check your
white blood cell count during treatment with BLINCYTO. Tell your healthcare
provider right away if you get a fever.
· Abnormal liver blood tests. Your
healthcare provider will do blood tests to check your liver before you start
BLINCYTO and during treatment with BLINCYTO.
· Inflammation of the pancreas
(pancreatitis). Pancreatitis may happen in people treated with BLINCYTO
and corticosteroids. It may be severe and lead to death. Tell your healthcare
provider right away if you have severe stomach-area pain that does not go away.
The pain may happen with or without nausea and vomiting.
The most common side effects of BLINCYTO include:
· infections
· fever
· headache
· low red blood cell count
(anemia)
· low platelet count (thrombocytopenia)
· reactions related to infusion
of the medicine such as face swelling, low blood pressure, and high blood pressure (infusion-related
reactions)
These are not all the possible side effects of BLINCYTO.
Call your doctor for medical advice about side effects. You
may report side effects to FDA at 1-800-FDA-1088.
How should I store BLINCYTO?
Intravenous (IV) bags containing BLINCYTO for infusion will
arrive in a special package.
· Do not open the package.
· Do not freeze the package.
· The package containing BLINCYTO
will be opened by your healthcare provider and stored in the refrigerator at
36°F to 46°F (2°C to 8°C) for up to 8 days.
· Do not throw away (dispose of)
any BLINCYTO in your household trash. Talk with your healthcare provider about
disposal of BLINCYTO and used supplies.
Keep BLINCYTO and all medicines out of reach of children.
General information about safe and effective use of
BLINCYTO
Medicines are sometimes prescribed for purposes other than
those listed in a Medication Guide. Do not use BLINCYTO for a condition for
which it was not prescribed. Do not give BLINCYTO to other people even if they
have the same symptoms that you have. It may harm them. You can ask your
pharmacist or healthcare provider for information about BLINCYTO that is
written for health professionals.
What are the ingredients in BLINCYTO?
Active ingredient: blinatumomab
Inactive ingredients: citric acid monohydrate, lysine
hydrochloride, polysorbate 80, trehalose dihydrate, sodium hydroxide and
preservative-free sterile water for injection.
