通用中文 | 注射用比伐芦定 | 通用外文 | Bivalirudin |
品牌中文 | 品牌外文 | Angiomax | |
其他名称 | 比瓦尔丁 Angiox | ||
公司 | BAXTER(BAXTER) | 产地 | 美国(USA) |
含量 | 250mg | 包装 | 10支/盒 |
剂型给药 | 注射液 粉针剂 | 储存 | 室温 |
适用范围 | 抗凝药,不稳定型心绞痛患者接受PTCA术;经皮干预冠脉的急性缺血性并发症 |
通用中文 | 注射用比伐芦定 |
通用外文 | Bivalirudin |
品牌中文 | |
品牌外文 | Angiomax |
其他名称 | 比瓦尔丁 Angiox |
公司 | BAXTER(BAXTER) |
产地 | 美国(USA) |
含量 | 250mg |
包装 | 10支/盒 |
剂型给药 | 注射液 粉针剂 |
储存 | 室温 |
适用范围 | 抗凝药,不稳定型心绞痛患者接受PTCA术;经皮干预冠脉的急性缺血性并发症 |
【英文药名】Angiomax(Bivalirudin Inj)
【中文药名】比伐卢定注射剂
【药物剂型】注射剂(冻干粉剂):250mg。
【药理作用】
本品是一种合成的抗凝药,是天然产生的水蛭素的类似物,是由20个氨基酸组成的多肽,能高亲和地与凝血酶结合而特异地抑制凝血酶活性,抑制凝血酶所催化和诱导的反应。比伐卢定不仅能与血浆游离的凝血酶结合,也能与血块相连的凝血酶结合,此结合是可逆的,且不需要AT-Ⅲ的存在。比伐卢定具有较强的抗凝作用,对多种动物动脉和静脉模型均有抗血栓作用。比伐卢定可使部分凝血活酶时间(APTT)、凝血酶时间(PT)和活化凝血时间(ACT)延长。
【药动学】
比伐卢定不结合于血浆蛋白(除了凝血酶),在静推比伐卢定时,剂量与血浆浓度呈线性关系。静推比伐卢定1mg/kg和静脉滴注每小时2.5mg/kg 4h后,比伐卢定血浆浓度达稳态。比伐卢定是通过肾脏以蛋白水解方式中从血浆中清除,肾功能正常者的清除半衰期约为25min,中、重度的肾功能不全患者的清除半衰期延长。25%的比伐卢定可被透析掉。须监测APTT。本品静脉注射后,立即出现抗凝作用,可见到PT,APTT的时间延长。停药后1~2h,PT就可恢复正常范围。
【适应症】
不稳定型心绞痛患者接受PTCA术;经皮干预冠脉的急性缺血性并发症。
【用法用量】
为了减少接受经皮经腔冠状动脉成形术(PTCA)的不稳定型心绞痛患者发生急性缺血性并发症,建议在进行PTCA之前,立即静脉注射本品1mg/kg,继而以每小时2.5mg/kg的速度持续输注本品4h。如有必要,再以每小时0.2mg/kg的速度持续输注20h。同时,每天可以合用阿司匹林325mg。
【如何购买】
好医友美国药房提供专科药物、处方药物、非处方药物、药物配置、药物注射以及各类非住院患者的药物分发、咨询、配送等各项服务。美国是医药分开的国家,药房全部实行严格的处方药与非处方药分类管理。对处方药的销售,必须凭美国医生(电子/纸质)处方。如今国内患者可以依托科技,实现远程的病历交互,由美国医生根据患者病情开具电子处方,以正规渠道在美国药房购买到处方药。
【禁忌症】
1.对本品过敏者、哺乳者禁用。
2.对任何出血患者禁用。
【注意事项】
用药后,尤其是中、重度的肾功能不全患者应注意监测APTT值。孕妇及哺乳期妇女用药,由于对妊娠及哺乳期妇女没有足够的临床研究,对妊娠妇女只有在必须用药时才可应用。动物研究显示,本品可进入乳汁,所以应以用药对哺乳期妇女的重要性来决定是停止哺乳还是停药。儿童用药,尚没有儿童用药的安全性资料。
老年患者用药,没有必要对老年人调整剂量。药物过量,若应用比伐卢定过量,无特效药物纠正,须停用比伐卢定。出血风险增高者慎用,中重度肾功能不全者不必减少开始的用量,但应减少最后20h的输注用量,并监测激活凝血时间(ACT)。也可根据肾小球滤过率(GRF)调整剂量。GRF为每分钟60~90ml者使用常用量,每分钟30~59ml者减量20%,每分钟10~29ml者减量60%;依赖透析者减量90%。
【不良反应】
出血为主要的不良反应。也可出现背痛、恶心、低血压和头痛。过敏反应的发生率为14%。用比伐卢定治疗不稳定型心绞痛患者停药后可出现心绞痛,及时给予足量阿司匹林可避免。注射部位疼痛、失眠、呕吐、骨盆痛、焦虑、心动过缓、厌食、腹痛、发热和神经过敏也有报道。
【药物相应作用】
临床用华法林治疗时以凝血时间(PT)作为监测,比伐卢定可延长PT,故两药合用可影响华法林的治疗监测。肝素和阿加曲班均延长APTT。阿司匹林与比伐卢定合用不影响阿加曲班的血浆浓度。抑制凝血的药物,除阿司匹林外,与本品合用的安全性尚未确定。而与阿司匹林合用,可加强抗凝作用,亦应常查PT和APTT,防止出血发生。
【英文药名】Angiomax(Bivalirudin Inj)
【中文药名】比伐卢定注射剂
【药物剂型】注射剂(冻干粉剂):250mg。
【药理作用】
本品是一种合成的抗凝药,是天然产生的水蛭素的类似物,是由20个氨基酸组成的多肽,能高亲和地与凝血酶结合而特异地抑制凝血酶活性,抑制凝血酶所催化和诱导的反应。比伐卢定不仅能与血浆游离的凝血酶结合,也能与血块相连的凝血酶结合,此结合是可逆的,且不需要AT-Ⅲ的存在。比伐卢定具有较强的抗凝作用,对多种动物动脉和静脉模型均有抗血栓作用。比伐卢定可使部分凝血活酶时间(APTT)、凝血酶时间(PT)和活化凝血时间(ACT)延长。
【药动学】
比伐卢定不结合于血浆蛋白(除了凝血酶),在静推比伐卢定时,剂量与血浆浓度呈线性关系。静推比伐卢定1mg/kg和静脉滴注每小时2.5mg/kg 4h后,比伐卢定血浆浓度达稳态。比伐卢定是通过肾脏以蛋白水解方式中从血浆中清除,肾功能正常者的清除半衰期约为25min,中、重度的肾功能不全患者的清除半衰期延长。25%的比伐卢定可被透析掉。须监测APTT。本品静脉注射后,立即出现抗凝作用,可见到PT,APTT的时间延长。停药后1~2h,PT就可恢复正常范围。
【适应症】
不稳定型心绞痛患者接受PTCA术;经皮干预冠脉的急性缺血性并发症。
【用法用量】
为了减少接受经皮经腔冠状动脉成形术(PTCA)的不稳定型心绞痛患者发生急性缺血性并发症,建议在进行PTCA之前,立即静脉注射本品1mg/kg,继而以每小时2.5mg/kg的速度持续输注本品4h。如有必要,再以每小时0.2mg/kg的速度持续输注20h。同时,每天可以合用阿司匹林325mg。
【如何购买】
好医友美国药房提供专科药物、处方药物、非处方药物、药物配置、药物注射以及各类非住院患者的药物分发、咨询、配送等各项服务。美国是医药分开的国家,药房全部实行严格的处方药与非处方药分类管理。对处方药的销售,必须凭美国医生(电子/纸质)处方。如今国内患者可以依托科技,实现远程的病历交互,由美国医生根据患者病情开具电子处方,以正规渠道在美国药房购买到处方药。
【禁忌症】
1.对本品过敏者、哺乳者禁用。
2.对任何出血患者禁用。
【注意事项】
用药后,尤其是中、重度的肾功能不全患者应注意监测APTT值。孕妇及哺乳期妇女用药,由于对妊娠及哺乳期妇女没有足够的临床研究,对妊娠妇女只有在必须用药时才可应用。动物研究显示,本品可进入乳汁,所以应以用药对哺乳期妇女的重要性来决定是停止哺乳还是停药。儿童用药,尚没有儿童用药的安全性资料。
老年患者用药,没有必要对老年人调整剂量。药物过量,若应用比伐卢定过量,无特效药物纠正,须停用比伐卢定。出血风险增高者慎用,中重度肾功能不全者不必减少开始的用量,但应减少最后20h的输注用量,并监测激活凝血时间(ACT)。也可根据肾小球滤过率(GRF)调整剂量。GRF为每分钟60~90ml者使用常用量,每分钟30~59ml者减量20%,每分钟10~29ml者减量60%;依赖透析者减量90%。
【不良反应】
出血为主要的不良反应。也可出现背痛、恶心、低血压和头痛。过敏反应的发生率为14%。用比伐卢定治疗不稳定型心绞痛患者停药后可出现心绞痛,及时给予足量阿司匹林可避免。注射部位疼痛、失眠、呕吐、骨盆痛、焦虑、心动过缓、厌食、腹痛、发热和神经过敏也有报道。
【药物相应作用】
临床用华法林治疗时以凝血时间(PT)作为监测,比伐卢定可延长PT,故两药合用可影响华法林的治疗监测。肝素和阿加曲班均延长APTT。阿司匹林与比伐卢定合用不影响阿加曲班的血浆浓度。抑制凝血的药物,除阿司匹林外,与本品合用的安全性尚未确定。而与阿司匹林合用,可加强抗凝作用,亦应常查PT和APTT,防止出血发生。
Dosage Form: injection, powder, lyophilized, for solution
Indications and Usage for BivalirudinPercutaneous Transluminal Coronary Angioplasty (PTCA)
Bivalirudin for Injection is indicated for use as an anticoagulant in patients with unstable angina undergoing percutaneous transluminal coronary angioplasty (PTCA).
Percutaneous Coronary Intervention (PCI)Bivalirudin for Injection with provisional use of glycoprotein IIb/IIIa inhibitor (GPI) as listed in the REPLACE-2 trial [see Clinical Studies (14.1)] is indicated for use as an anticoagulant in patients undergoing percutaneous coronary intervention (PCI).
Bivalirudin for Injection is indicated for patients with, or at risk of, heparin induced thrombocytopenia (HIT) or heparin induced thrombocytopenia and thrombosis syndrome (HITTS) undergoing PCI.
Use with AspirinBivalirudin for Injection in these indications is intended for use with aspirin and has been studied only in patients receiving concomitant aspirin [see Dosage and Administration (2.1) and Clinical Studies (14.1)].
Limitation of UseThe safety and effectiveness of Bivalirudin for Injection have not been established in patients with acute coronary syndromes who are not undergoing PTCA or PCI.
Bivalirudin Dosage and AdministrationRecommended DoseBivalirudin for Injection is for intravenous administration only.
Bivalirudin for Injection is intended for use with aspirin (300 to 325 mg daily) and has been studied only in patients receiving concomitant aspirin.
For patients who do not have HIT/HITTS
The recommended dose of Bivalirudin for Injection is an intravenous (IV) bolus dose of 0.75 mg/kg, followed immediately by an infusion of 1.75 mg/kg/h for the duration of the PCI/PTCA procedure. Five min after the bolus dose has been administered, an activated clotting time (ACT) should be performed and an additional bolus of 0.3 mg/kg should be given if needed.
GPI administration should be considered in the event that any of the conditions listed in the REPLACE-2 clinical trial description [see Clinical Studies (14.1)] is present.
For patients who have HIT/HITTS
The recommended dose of Bivalirudin for Injection in patients with HIT/HITTS undergoing PCI is an IV bolus of 0.75 mg/kg. This should be followed by a continuous infusion at a rate of 1.75 mg/kg/h for the duration of the procedure.
For ongoing treatment post-procedure
Bivalirudin for Injection infusion may be continued following PCI/PTCA for up to 4 hours post-procedure at the discretion of the treating physician.
In patients with ST segment elevation myocardial infarction (STEMI) continuation of the Bivalirudin for Injection infusion at a rate of 1.75 mg/kg/h following PCI/PTCA for up to 4 hours post-procedure should be considered to mitigate risk of stent thrombosis. [see Warnings and Precautions (5.2)].
After four hours, an additional IV infusion of Bivalirudin for Injection may be initiated at a rate of 0.2 mg/kg/h (low-rate infusion), for up to 20 hours, if needed.
Dosing in Renal ImpairmentNo reduction in the bolus dose is needed for any degree of renal impairment. The infusion dose of Bivalirudin for Injection may need to be reduced, and anticoagulant status monitored in patients with renal impairment. Patients with moderate renal impairment (30 to 59 mL/min) should receive an infusion of 1.75 mg/kg/h. If the creatinine clearance is less than 30 mL/min, reduction of the infusion rate to 1 mg/kg/h should be considered. If a patient is on hemodialysis, the infusion rate should be reduced to 0.25 mg/kg/h [see Use in Specific Populations (8.6)].
Instructions for Administration
Bivalirudin for Injection is intended for intravenous bolus injection and continuous infusion after reconstitution and dilution. To each 250 mg vial, add 5 mL of Sterile Water for Injection, USP. Gently swirl until all material is dissolved. Next, withdraw and discard 5 mL from a 50 mL infusion bag containing 5% Dextrose in Water or 0.9% Sodium Chloride for Injection. Then add the contents of the reconstituted vial to the infusion bag containing 5% Dextrose in Water or 0.9% Sodium Chloride for Injection to yield a final concentration of 5 mg/mL (e.g., 1 vial in 50 mL; 2 vials in 100 mL; 5 vials in 250 mL). The dose to be administered is adjusted according to the patient’s weight (see Table 1).
If the low-rate infusion is used after the initial infusion, a lower concentration bag should be prepared. In order to prepare this lower concentration, reconstitute the 250 mg vial with 5 mL of Sterile Water for Injection, USP. Gently swirl until all material is dissolved. Next, withdraw and discard 5 mL from a 500 mL infusion bag containing 5% Dextrose in Water or 0.9% Sodium Chloride for Injection. Then add the contents of the reconstituted vial to the infusion bag containing 5% Dextrose in Water or 0.9% Sodium Chloride for Injection to yield a final concentration of 0.5 mg/mL. The infusion rate to be administered should be selected from the right-hand column in Table 1.
Table 1: Dosing Table
|
|
|
|
|
|
|
|
43 to 47 |
7 |
16 |
18 |
48 to 52 |
7.5 |
17.5 |
20 |
53 to 57 |
8 |
19 |
22 |
58 to 62 |
9 |
21 |
24 |
63 to 67 |
10 |
23 |
26 |
68 to 72 |
10.5 |
24.5 |
28 |
73 to 77 |
11 |
26 |
30 |
78 to 82 |
12 |
28 |
32 |
83 to 87 |
13 |
30 |
34 |
88 to 92 |
13.5 |
31.5 |
36 |
93 to 97 |
14 |
33 |
38 |
98 to 102 |
15 |
35 |
40 |
103 to 107 |
16 |
37 |
42 |
108 to 112 |
16.5 |
38.5 |
44 |
113 to 117 |
17 |
40 |
46 |
118 to 122 |
18 |
42 |
48 |
123 to 127 |
19 |
44 |
50 |
128 to 132 |
19.5 |
45.5 |
52 |
133 to 137 |
20 |
47 |
54 |
138 to 142 |
21 |
49 |
56 |
143 to 147 |
22 |
51 |
58 |
148 to 152 |
22.5 |
52.5 |
60 |
Bivalirudin for Injection should be administered via an intravenous line. No incompatibilities have been observed with glass bottles or polyvinyl chloride bags and administration sets. The following drugs should not be administered in the same intravenous line with Bivalirudin for Injection, since they resulted in haze formation, microparticulate formation, or gross precipitation when mixed with Bivalirudin for Injection: alteplase, amiodarone HCl, amphotericin B, chlorpromazine HCl, diazepam, prochlorperazine edisylate, reteplase, streptokinase, and vancomycin HCl. Dobutamine was compatible at concentrations up to 4 mg/mL but incompatible at a concentration of 12.5 mg/mL.
Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration. Preparations of Bivalirudin for Injection containing particulate matter should not be used. Reconstituted material will be a clear to slightly opalescent, colorless to slightly yellow solution.
Storage after ReconstitutionDo not freeze reconstituted or diluted Bivalirudin for Injection. Reconstituted material may be stored at 2 to 8ºC for up to 24 hours. Diluted Bivalirudin for Injection with a concentration of between 0.5 mg/mL and 5 mg/mL is stable at room temperature for up to 24 hours. Discard any unused portion of reconstituted solution remaining in the vial.
Dosage Forms and StrengthsFor injection: 250 mg of Bivalirudin in a single-dose vial for reconstitution. Each vial contains 250 mg of Bivalirudin equivalent to an average of 270 mg Bivalirudin trifluoroacetate*. Following reconstitution with Sterile Water for Injection, the product is a clear to opalescent, colorless to slightly yellow solution, pH 5 to 6.
*The range of Bivalirudin trifluoroacetate is 260 to 280 mg based on a range of trifluoroacetic acid composition of 1.0 to 2.2 equivalents.
ContraindicationsBivalirudin for Injection is contraindicated in patients with:
· Active major bleeding;
· Hypersensitivity (e.g., anaphylaxis) to Bivalirudin or its components [see Adverse Reactions (6.3)].
Warnings and PrecautionsBleeding EventsAlthough most bleeding associated with the use of Bivalirudin in PCI/PTCA occurs at the site of arterial puncture, hemorrhage can occur at any site. An unexplained fall in blood pressure or hematocrit should lead to serious consideration of a hemorrhagic event and cessation of Bivalirudin administration [see Adverse Reactions (6.1)]. Bivalirudin should be used with caution in patients with disease states associated with an increased risk of bleeding.
Acute Stent Thrombosis in Patients with STEMI undergoing PCIAcute stent thrombosis (AST) (<4 hours) has been observed at a greater frequency in Bivalirudin for Injection treated patients (1.2%, 36/2,889) compared to heparin treated patients (0.2%, 6/2,911) with STEMI undergoing primary PCI. Among patients who experienced an AST, one fatality (0.03%) occurred in a Bivalirudin treated patient and one fatality (0.03%) in a heparin treated patient. These patients have been managed by Target Vessel Revascularization (TVR). Patients should remain for at least 24 hours in a facility capable of managing ischemic complications and should be carefully monitored following primary PCI for signs and symptoms consistent with myocardial ischemia.
Coronary Artery BrachytherapyAn increased risk of thrombus formation, including fatal outcomes, has been associated with the use of Bivalirudin for Injection in gamma brachytherapy.
If a decision is made to use Bivalirudin for Injection during brachytherapy procedures, maintain meticulous catheter technique, with frequent aspiration and flushing, paying special attention to minimizing conditions of stasis within the catheter or vessels [see Adverse Reactions (6.3)].
Laboratory Test InterferenceBivalirudin affects International Normalized Ratio (INR), therefore INR measurements made in patients who have been treated with Bivalirudin for Injection may not be useful for determining the appropriate dose of warfarin.
Adverse Reactions
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.
Bleeding
In 6,010 patients undergoing PCI treated in the REPLACE-2 trial, Bivalirudin patients exhibited statistically significantly lower rates of bleeding, transfusions, and thrombocytopenia as noted in Table 2.
Table 2: Major Hematologic Outcomes REPLACE-2 (Safety Population)
|
|
|
|
|
|
|
|
|
|
||
|
|
|
|
|
|
|
||
|
|
|
|
|
|
|
||
|
|
|
|
||
|
|
|
|
|
|
|
||
|
|
|
|
|
|
1 GPIs were administered to 7.2% of patients in the Bivalirudin with provisional GPI group.
2 Defined as the occurrence of any of the following: intracranial bleeding, retroperitoneal bleeding, a transfusion of ≥ 2 units of blood/blood products, a fall in hemoglobin > 4g/dL, whether or not bleeding site is identified, spontaneous or non-spontaneous blood loss with a decrease in hemoglobin >3g/dL.
3 Defined as observed bleeding that does not meet the criteria for major hemorrhage.
4 TIMI major bleeding is defined as intracranial, or a fall in adjusted Hgb >5g/dL or Hct of >15%: TIMI minor bleeding is defined as a fall in adjusted Hgb of 3 to <5 g/dL or a fall in adjusted Hct of 9 to <15%, with a bleeding site such as hematuria, hematemesis, hematomas, retroperitoneal bleeding or a decrease in Hgb of >4 g/dL with no bleeding site.
5 If <100,000 and >25% reduction from baseline, or <50,000.
In 4,312 patients undergoing PTCA for treatment of unstable angina in 2 randomized, double-blind studies comparing Bivalirudin to heparin, Bivalirudin patients exhibited lower rates of major bleeding and lower requirements for blood transfusions. The incidence of major bleeding is presented in Table 3. The incidence of major bleeding was lower in the Bivalirudin group than in the heparin group.
Table 3: Major Bleeding and Transfusions in BAT Trial (all patients)*
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
* No monitoring of ACT (or PTT) was done after a target ACT was achieved.
1 Major hemorrhage was defined as the occurrence of any of the following, intracranial bleeding, retroperitoneal bleeding, clinically overt bleeding with a decrease in hemoglobin ≥ 3 g/dL or leading to a transfusion of > 2 units of blood. This table includes data from the entire hospitalization period.
In the AT-BAT study, of the 51 patients with HIT/HITTS, 1 patient who did not undergo PCI had major bleeding during CABG on the day following angiography. Nine patients had minor bleeding (mostly due to access site bleeding), and 2 patients developed thrombocytopenia.
Other Adverse Reactions
Adverse reactions, other than bleeding, observed in clinical trials were similar between the Bivalirudin treated patients and the control groups.
Adverse reactions (related adverse events) seen in clinical studies in patients undergoing PCI and PTCA are shown in Tables 4 and 5.
Table 4: Most Frequent (>0.2%) Treatment-related Adverse Events (reactions)(through 30 days) in the REPLACE-2 Safety Population
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
1 Note: A patient could have been more than one event in any category.
Abbreviation: AE = Adverse Event.
Table 5: Adverse Reactions Other Than Bleeding Occurring In ≥ 5% of Patients in Either Treatment Group in BAT Trial
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
Serious, non-bleeding adverse events were experienced in 2% of 2,161 Bivalirudin-treated patients and 2% of 2,151 heparin-treated patients. The following individual serious non-bleeding adverse events were rare (>0.1% to <1%) and similar in incidence between Bivalirudin- and heparin-treated patients. These events are listed by body system: Body as a Whole: fever, infection, sepsis; Cardiovascular: hypotension, syncope, vascular anomaly, ventricular fibrillation; Nervous: cerebral ischemia, confusion, facial paralysis; Respiratory: lung edema; Urogenital: kidney failure, oliguria. In the BAT trial, there was no causality assessment for adverse events.
Immunogenicity/Re-ExposureIn in vitro studies, Bivalirudin exhibited no platelet aggregation response against sera from patients with a history of HIT/HITTS.
Among 494 subjects who received Bivalirudin in clinical trials and were tested for antibodies, 2 subjects had treatment-emergent positive Bivalirudin antibody tests. Neither subject demonstrated clinical evidence of allergic or anaphylactic reactions and repeat testing was not performed. Nine additional patients who had initial positive tests were negative on repeat testing.
Postmarketing ExperienceBecause postmarketing adverse 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.
The following adverse reactions have been identified during postapproval use of Bivalirudin: fatal bleeding; hypersensitivity and allergic reactions including reports of anaphylaxis; lack of anticoagulant effect; thrombus formation during PCI with and without intracoronary brachytherapy, including reports of fatal outcomes; pulmonary hemorrhage; cardiac tamponade; and INR increased.
Drug InteractionsIn clinical trials in patients undergoing PCI/PTCA, co-administration of Bivalirudin with heparin, warfarin, thrombolytics, or GPIs was associated with increased risks of major bleeding events compared to patients not receiving these concomitant medications.
There is no experience with co-administration of Bivalirudin and plasma expanders such as dextran.
USE IN SPECIFIC POPULATIONSPregnancyPregnancy Category B
Reproductive studies have been performed in rats at subcutaneous doses up to 150 mg/kg/day, (1.6 times the maximum recommended human dose based on body surface area) and rabbits at subcutaneous doses up to 150 mg/kg/day (3.2 times the maximum recommended human dose based on body surface area). These studies revealed no evidence of impaired fertility or harm to the fetus attributable to Bivalirudin. There are, however, no adequate and well-controlled studies in pregnant women. Because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed.
Bivalirudin is intended for use with aspirin [see Indications and Usage (1.3)]. Because of possible adverse effects on the neonate and the potential for increased maternal bleeding, particularly during the third trimester, Bivalirudin and aspirin should be used together during pregnancy only if clearly needed.
Nursing MothersIt is not known whether Bivalirudin is excreted in human milk. Because many drugs are excreted in human milk, caution should be exercised when Bivalirudin is administered to a nursing woman.
Pediatric UseThe safety and effectiveness of Bivalirudin in pediatric patients have not been established.
Geriatric UseIn studies of patients undergoing PCI, 44% were ≥65 years of age and 12% of patients were ≥75 years old. Elderly patients experienced more bleeding events than younger patients. Patients treated with Bivalirudin experienced fewer bleeding events in each age stratum, compared to heparin.
Renal ImpairmentThe disposition of Bivalirudin was studied in PTCA patients with mild, moderate and severe renal impairment. The clearance of Bivalirudin was reduced approximately 20% in patients with moderate and severe renal impairment and was reduced approximately 80% in dialysis-dependent patients [see Clinical Pharmacology (12.3)]. The infusion dose of Bivalirudin may need to be reduced, and anticoagulant status monitored in patients with renal impairment [see Dosage and Administration (2.2)].
OverdosageCases of overdose of up to 10 times the recommended bolus or continuous infusion dose of Bivalirudin have been reported in clinical trials and in postmarketing reports. A number of the reported overdoses were due to failure to adjust the infusion dose of Bivalirudin in persons with renal dysfunction including persons on hemodialysis [see Dosage and Administration (2.2)]. Bleeding, as well as deaths due to hemorrhage, have been observed in some reports of overdose. In cases of suspected overdosage, discontinue Bivalirudin immediately and monitor the patient closely for signs of bleeding. There is no known antidote to Bivalirudin. Bivalirudin is hemodialyzable [see Clinical Pharmacology (12.3)].
Bivalirudin DescriptionBivalirudin for Injection contains Bivalirudin which is a specific and reversible direct thrombin inhibitor. Bivalirudin is a synthetic, 20 amino acid peptide, with the chemical name of D-phenylalanyl-L-prolyl-L-arginyl-L-prolyl-glycyl-glycyl-glycyl-glycyl-L-asparagyl-glycyl-L-aspartyl-L-phenylalanyl-L-glutamyl-L-glutamyl-L-isoleucyl-L-prolyl-L-glutamyl-L-glutamyl-L-tyrosyl-L-leucine. The active pharmaceutical ingredient is in the form of Bivalirudin trifluoroacetate as a white to off-white powder. The chemical name for Bivalirudin trifluoroacetate is D-phenylalanyl-L-prolyl-L-arginyl-L-prolyl-glycyl-glycyl-glycyl-glycyl-L-asparagyl-glycyl-L-aspartyl-L-phenylalanyl-L-glutamyl-L-glutamyl-L-isoleucyl-L-prolyl-L-glutamyl-L-glutamyl-L-tyrosyl-L-leucine trifluoroacetate (Figure 1). The molecular weight of Bivalirudin is 2,180 daltons (anhydrous free base peptide).
Figure 1. Structural formula for Bivalirudin trifluoroacetate
Bivalirudin for Injection is supplied as a sterile white lyophilized cake, in single-dose vials. Each vial contains 250 mg Bivalirudin, equivalent to an average of 270 mg of Bivalirudin trifluoroactetate*, 125 mg mannitol, and sodium hydroxide to adjust the pH to 5 to 6 (equivalent of approximately 12.5 mg sodium). When reconstituted with Sterile Water for Injection, the product yields a clear to opalescent, colorless to slightly yellow solution, pH 5 to 6.
*The range of Bivalirudin trifluoroacetate is 260 mg to 280 mg based on a range of trifluoroacetic acid composition of 1.0 to 2.2 equivalents.
Bivalirudin - Clinical PharmacologyMechanism of ActionBivalirudin directly inhibits thrombin by specifically binding both to the catalytic site and to the anion-binding exosite of circulating and clot-bound thrombin. Thrombin is a serine proteinase that plays a central role in the thrombotic process, acting to cleave fibrinogen into fibrin monomers and to activate Factor XIII to Factor XIIIa, allowing fibrin to develop a covalently cross-linked framework which stabilizes the thrombus; thrombin also activates Factors V and VIII, promoting further thrombin generation, and activates platelets, stimulating aggregation and granule release. The binding of Bivalirudin to thrombin is reversible as thrombin slowly cleaves the Bivalirudin-Arg3-Pro4 bond, resulting in recovery of thrombin active site functions.
In in vitro studies, Bivalirudin inhibited both soluble (free) and clot-bound thrombin, was not neutralized by products of the platelet release reaction, and prolonged the activated partial thromboplastin time (aPTT), thrombin time (TT), and prothrombin time (PT) of normal human plasma in a concentration-dependent manner. The clinical relevance of these findings is unknown.
PharmacodynamicsIn healthy volunteers and patients (with ≥70% vessel occlusion undergoing routine PTCA), Bivalirudin exhibited dose- and concentration-dependent anticoagulant activity as evidenced by prolongation of the ACT, aPTT, PT, and TT. Intravenous administration of Bivalirudin produces an immediate anticoagulant effect. Coagulation times return to baseline approximately 1 hour following cessation of Bivalirudin administration.
In 291 patients with ≥70% vessel occlusion undergoing routine PTCA, a positive correlation was observed between the dose of Bivalirudin and the proportion of patients achieving ACT values of 300 sec or 350 sec. At a Bivalirudin dose of 1 mg/kg IV bolus plus 2.5 mg/kg/h IV infusion for 4 hours, followed by 0.2 mg/kg/h, all patients reached maximal ACT values >300 sec.
PharmacokineticsBivalirudin exhibits linear pharmacokinetics following IV administration to patients undergoing PTCA. In these patients, a mean steady state Bivalirudin concentration of 12.3 ± 1.7 mcg/mL is achieved following an IV bolus of 1 mg/kg and a 4-hour 2.5 mg/kg/h IV infusion. Bivalirudin does not bind to plasma proteins (other than thrombin) or to red blood cells. Bivalirudin is cleared from plasma by a combination of renal mechanisms and proteolytic cleavage, with a half-life in patients with normal renal function of 25 min.
The disposition of Bivalirudin was studied in PTCA patients with mild, moderate, and severe renal impairment. Drug elimination was related to glomerular filtration rate (GFR). Total body clearance was similar for patients with normal renal function and with mild renal impairment (60 to 89 mL/min). Clearance was reduced in patients with moderate and severe renal impairment and in dialysis-dependent patients (see Table 6 for pharmacokinetic parameters).
Bivalirudin is hemodialyzable, with approximately 25% cleared by hemodialysis.
Table 6: PK Parameters in Patients with Renal Impairment*
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
*The ACT should be monitored in renally-impaired patients.
No long-term studies in animals have been performed to evaluate the carcinogenic potential of Bivalirudin. Bivalirudin displayed no genotoxic potential in the in vitro bacterial cell reverse mutation assay (Ames test), the in vitro Chinese hamster ovary cell forward gene mutation test (CHO/HGPRT), the in vitro human lymphocyte chromosomal aberration assay, the in vitro rat hepatocyte unscheduled DNA synthesis (UDS) assay, and the in vivo rat micronucleus assay. Fertility and general reproductive performance in rats were unaffected by subcutaneous doses of Bivalirudin up to 150 mg/kg/day, about 1.6 times the dose on a body surface area basis (mg/m2) of a 50 kg person given the maximum recommended dose of 15 mg/kg/day.
Clinical StudiesPCI/PTCABivalirudin has been evaluated in five randomized, controlled interventional cardiology trials reporting 11,422 patients. Stents were deployed in 6,062 of the patients in these trials – mainly in trials performed since 1995. Percutaneous transluminal coronary angioplasty, atherectomy or other procedures were performed in the remaining patients.
REPLACE-2 Trial
This was a randomized, double-blind, multicenter study reporting 6,002 (intent-to-treat) patients undergoing PCI. Patients were randomized to treatment with Bivalirudin with the “provisional” use of platelet glycoprotein IIb/IIIa inhibitor (GPI) or heparin plus planned use of GPI. GPIs were added on a “provisional” basis to patients who were randomized to Bivalirudin in the following circumstances:
• decreased TIMI flow (0 to 2) or slow reflow;
• dissection with decreased flow;
• new or suspected thrombus;
• persistent residual stenosis;
• distal embolization;
• unplanned stent;
• suboptimal stenting;
• side branch closure;
• abrupt closure; clinical instability; and
• prolonged ischemia.
During the study, one or more of these circumstances occurred in 10.9% of patients in the Bivalirudin with provisional GPI arm. GPIs were administered to 7.2% of patients in the Bivalirudin with provisional GPI arm (66.8% of eligible patients).
Patients ranged in age from 25 to 95 years (median, 63); weight ranged from 35 to 199 kg (median 85.5); 74.4% were male and 25.6% were female. Indications for PCI included unstable angina (35% of patients), myocardial infarction within 7 days prior to intervention (8% of patients), stable angina (25%), positive ischemic stress test (24%), and other not specified indications (8%). Stents were deployed in 85% of patients. Ninety-nine percent of patients received aspirin and 86% received thienopyridines prior to study treatment.
Bivalirudin was administered as a 0.75 mg/kg bolus followed by a 1.75 mg/kg/h infusion for the duration of the procedure. The activated clotting time (ACT – measured by a Hemochron® device) was measured 5 min after the first bolus of study medication. If the ACT was < 225 seconds, an additional bolus of 0.3 mg/kg was given. At investigator discretion, the infusion could be continued following the procedure for up to 4 hours. The median infusion duration was 44 min. Heparin was administered as a 65 U/kg bolus. The activated clotting time (ACT – measured by a Hemochron®device) was measured 5 min after the first bolus of study medication. If the ACT was < 225 seconds, an additional bolus of 20 units/kg was given. GPIs (either abciximab or eptifibatide) were given according to manufacturers’ instructions. Both randomized groups could be given “provisional” treatments during the PCI at investigator discretion, but under double-blind conditions. “Provisional” treatment with GPI was requested in 5.2% of patients randomized to heparin plus GPI (they were given placebo) and 7.2% patients randomized to Bivalirudin with provisional GPI (they were given abciximab or eptifibatide according to pre-randomization investigator choice and patient stratification).
The percent of patients reaching protocol-specified levels of anticoagulation was greater in the Bivalirudin with provisional GPI group than in the heparin plus GPI group. For patients randomized to Bivalirudin with provisional GPI, the median 5 min ACT was 358 sec (interquartile range 320 to 400 sec) and the ACT was < 225 sec in 3%. For patients randomized to heparin plus GPI, the median 5 min ACT was 317 sec (interquartile range 263 to 373 sec) and the ACT was < 225 sec in 12%. At the end of the procedure, median ACT values were 334 sec (Bivalirudin group) and 276 sec (heparin plus GPI group).
For the composite endpoint of death, MI, or urgent revascularization adjudicated under double-blind conditions, the frequency was higher (7.6%) (95% confidence interval 6.7% to 8.6%) in the Bivalirudin with “provisional” GPI arm when compared to the heparin plus GPI arm (7.1%) (95% confidence interval 6.1% to 8.0%). However, major hemorrhage was reported significantly less frequently in the Bivalirudin with provisional GPI arm (2.4%) compared to the heparin plus GPI arm (4.1%). Study outcomes are shown in Table 7.
Table 7: Incidences of Clinical Endpoints at 30 Days for REPLACE-2, a Randomized Double-blind Clinical Trial
|
|
|
|
||
|
|
|
|
|
|
|
|
|
|
|
|
|
||
|
|
|
1 Defined as intracranial bleeding, retroperitoneal bleeding, a transfusion of >2 units of blood/blood products, a fall in Hgb >4 g/dL, whether or not bleeding site is identified, spontaneous or non-spontaneous blood loss with a decrease in Hgb >3 g/dL.
2 p-value <0.001 between groups.
At 12 months’ follow-up, mortality was 1.9% among patients randomized to Bivalirudin with “provisional” GPIs and 2.5% among patients randomized to heparin plus GPI.
Bivalirudin Angioplasty Trial (BAT)
Bivalirudin was evaluated in patients with unstable angina undergoing PTCA in two randomized, double-blind, multicenter studies with identical protocols. Patients must have had unstable angina defined as: (1) a new onset of severe or accelerated angina or rest pain within the month prior to study entry or (2) angina or ischemic rest pain which developed between four hours and two weeks after an acute myocardial infarction (MI). Overall, 4,312 patients with unstable angina, including 741 (17%) patients with post-MI angina, were treated in a 1:1 randomized fashion with Bivalirudin or heparin. Patients ranged in age from 29 to 90 (median 63) years, their weight was a median of 80 kg (39 to 120 kg), 68% were male, and 91% were Caucasian. Twenty-three percent of patients were treated with heparin within one hour prior to randomization. All patients were administered aspirin 300 to 325 mg prior to PTCA and daily thereafter. Patients randomized to Bivalirudin were started on an intravenous infusion of Bivalirudin (2.5 mg/kg/h). Within 5 min after starting the infusion, and prior to PTCA, a 1 mg/kg loading dose was administered as an intravenous bolus. The infusion was continued for 4 hours, then the infusion was changed under double-blinded conditions to Bivalirudin (0.2 mg/kg/h) for up to an additional 20 hours (patients received this infusion for an average of 14 hours). The ACT was checked at 5 min and at 45 min following commencement. If on either occasion the ACT was <350 sec, an additional double-blinded bolus of placebo was administered. The Bivalirudin dose was not titrated to ACT. Median ACT values were: ACT in sec (5th percentile to 95thpercentile): 345 sec (240 to 595 sec) at 5 min and 346 sec (range 269 to 583 sec) at 45 min after initiation of dosing. Patients randomized to heparin were given a loading dose (175 IU/kg) as an intravenous bolus 5 min before the planned procedure, with immediate commencement of an infusion of heparin (15 IU/kg/h). The infusion was continued for 4 hours. After 4 hours of infusion, the heparin infusion was changed under double-blinded conditions to heparin (15 IU/kg/h) for up to 20 additional hours. The ACT was checked at 5 min and at 45 min following commencement. If on either occasion the ACT was <350 sec, an additional double-blind bolus of heparin (60 IU/kg) was administered. Once the target ACT was achieved for heparin patients, no further ACT measurements were performed. All ACTs were determined with the Hemochron® device. The protocol allowed use of open-label heparin at the discretion of the investigator after discontinuation of blinded study medication, whether or not an endpoint event (procedural failure) had occurred. The use of open-label heparin was similar between Bivalirudin and heparin treatment groups (about 20% in both groups).
The studies were designed to demonstrate the safety and efficacy of Bivalirudin in patients undergoing PTCA as a treatment for unstable angina as compared with a control group of similar patients receiving heparin during and up to 24 hours after initiation of PTCA. The primary protocol endpoint was a composite endpoint called procedural failure, which included both clinical and angiographic elements measured during hospitalization. The clinical elements were: the occurrence of death, MI, or urgent revascularization, adjudicated under double-blind conditions. The angiographic elements were: impending or abrupt vessel closure. The protocol-specified safety endpoint was major hemorrhage.
The median duration of hospitalization was 4 days for both the Bivalirudin and the heparin treatment groups. The rates of procedural failure were similar in the Bivalirudin and heparin treatment groups. Study outcomes are shown in Table 8.
Table 8: Incidences of In-hospital Clinical Endpoints in BAT Trial Occurring within 7 Days
|
|
|
|
||
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
||
|
|
|
1 The protocol-specified primary endpoint (a composite of death or MI or clinical deterioration of cardiac origin requiring revascularization or placement of an aortic balloon pump or angiographic evidence of abrupt vessel closure).
2 Defined as: Q-wave MI; CK-MB elevation ≥2 x ULN, new ST- or T-wave abnormality, and chest pain ≥30 min; OR new LBBB with chest pain ≥30 min and/or elevated CK-MB enzymes; OR elevated CK-MB and new ST- or T-wave abnormality without chest pain; OR elevated CK-MB.
3 Defined as: any revascularization procedure, including angioplasty, CABG, stenting, or placement of an intra-aortic balloon pump.
4 Defined as the occurrence of any of the following: intracranial bleeding, retroperitoneal bleeding, clinically overt bleeding with a decrease in Hgb ≥3 g/dL or leading to a transfusion of ≥2 units of blood.
AT-BAT Trial
This was a single-group open-label study which enrolled 51 patients with heparin-induced thrombocytopenia (HIT) or heparin-induced thrombocytopenia and thrombosis syndrome (HITTS) undergoing PCI. Evidence for the diagnosis of HIT/HITTS was based on a clinical history of a decrease of platelets in patients after heparin administration [new diagnosis or history of clinically suspected or objectively documented HIT/HITTS defined as either: 1) HIT: positive heparin-induced platelet aggregation (HIPA) or other functional assay where the platelet count has decreased to <100,000/mL (minimum 30% from prior to heparin), or has decreased to <150,000/mL (minimum 40% from prior to heparin), or has decreased as above within hours of receiving heparin in a patient with a recent, previous exposure to heparin; 2) HITTS: thrombocytopenia as above plus arterial or venous thrombosis diagnosed by physician examination/laboratory and/or appropriate imaging studies]. Patients ranged in age from 48 to 89 years (median 70); weight ranged from 42 to 123 kg (median 76); 50% were male and 50% were female. Bivalirudin was administered as either 1 mg/kg bolus followed by 2.5 mg/kg/h (high dose in 28 patients) or 0.75 mg/kg bolus followed by a 1.75 mg/kg/h infusion (lower dose in 25 patients) for up to 4 hours. Ninety-eight percent of patients received aspirin, 86% received clopidogrel and 19% received GPIs.
The median ACT values at the time of device activation were 379 sec (high dose) and 317 sec (lower dose). Following the procedure, 48 of the 51 patients (94%) had TIMI grade 3 flow and stenosis <50%. One patient died during a bradycardic episode 46 hours after successful PCI, another patient required surgical revascularization, and one patient experienced no flow requiring a temporary intra-aortic balloon.
Two of the fifty-one patients with the diagnosis of HIT/HITTS developed thrombocytopenia after receiving Bivalirudin and GPIs.
How Supplied/Storage and Handling
Bivalirudin for Injection is supplied as a sterile, lyophilized powder in single-dose, glass vials. Each vial contains 250 mg of Bivalirudin equivalent to an average of 270 mg of Bivalirudin trifluoroacetate*.
*The range of Bivalirudin trifluoroacetate is 260 to 280 mg based on a range of trifluoroacetic acid composition of 1.0 to 2.2 equivalents.
Product |
NDC |
Strength |
|
PRX506210 |
63323-562-15 |
250 mg per vial |
250 mg single-dose vial, packaged in tens. |
Store Bivalirudin for Injection dosage units at 20° to 25°C (68° to 77°F) [see USP Controlled Room Temperature].
The container closure is not made with natural rubber latex.
Advise patients to watch carefully for any signs of bleeding or bruising and to report these to their health care provider when they occur.
Advise patients to discuss with their health care provider their use of any other medications, including over-the-counter medications or herbal products, prior to Bivalirudin use. Examples of other medications that should not be taken with Bivalirudin are warfarin and heparin.
The brand names mentioned in this document are the trademarks of their respective owners.
PREMIERProRx® is a registered trademark of Premier Healthcare Alliance, L.P., used under license.
Manufactured by:
Fresenius Kabi
Lake Zurich, IL 60047
www.fresenius-kabi.com/us
451563
Revised: September 2017
PACKAGE LABEL - PRINCIPAL DISPLAY - Bivalirudin for Injection 250 mg Single Dose Vial Label
NDC 63323-562-41
Bivalirudin for Injection
250 mg per vial
For intravenous use only.
For single-dose only.
Discard unused portion.
Rx only
PACKAGE LABEL - PRINCIPAL DISPLAY - Bivalirudin for Injection 250 mg Single Dose Vial Tray Label
NDC 63323-562-15
Bivalirudin for Injection
250 mg per vial
For intravenous use only.
10 Single-dose vials.
Discard unused portion.
Rx only
Bivalirudin Bivalirudin injection, powder, lyophilized, for solution |
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
|
|||||||||||||||||
Labeler - Fresenius Kabi USA, LLC (608775388) |
Establishment |
|||
Name |
Address |
ID/FEI |
Operations |
Fresenius Kabi USA, LLC |
|
023648251 |
MANUFACTURE(63323-562) |
Revised: 10/2017
Fresenius Kabi USA, LLC