通用中文 | 马法兰片 | 通用外文 | Melphalan |
品牌中文 | 品牌外文 | Alphalan | |
其他名称 | 印度马法兰 马法兰片、爱克兰片、美法仑片、Alkeran | ||
公司 | NATCO(NATCO) | 产地 | 印度(India) |
含量 | 2mg | 包装 | 25片/盒 |
剂型给药 | 片剂 口服 | 储存 | 室温 |
适用范围 | 对多发性骨髓瘤 对恶性淋巴瘤、乳腺癌、卵巢癌、精原细胞瘤、慢性白血病、真性红细胞增多症、儿童晚期神经母细胞瘤、甲状腺癌 黑色素瘤、软组织肉瘤和骨肉瘤 |
通用中文 | 马法兰片 |
通用外文 | Melphalan |
品牌中文 | |
品牌外文 | Alphalan |
其他名称 | 印度马法兰 马法兰片、爱克兰片、美法仑片、Alkeran |
公司 | NATCO(NATCO) |
产地 | 印度(India) |
含量 | 2mg |
包装 | 25片/盒 |
剂型给药 | 片剂 口服 |
储存 | 室温 |
适用范围 | 对多发性骨髓瘤 对恶性淋巴瘤、乳腺癌、卵巢癌、精原细胞瘤、慢性白血病、真性红细胞增多症、儿童晚期神经母细胞瘤、甲状腺癌 黑色素瘤、软组织肉瘤和骨肉瘤 |
以下资料仅供参考:
文案整理:Dr. Jasmine Ding
马发兰使用说明书:
请仔细阅读说明书并在医师指导下使用:
【商品名称】
通用名称: 马发兰
品牌名称:Alphalan
通用英文名称:Melphalan
其他名称:爱克兰片、美法仑片、Alkeran, 左旋苯丙氨酸氮芥,L-Sarcolysin,L-PAM。
【成分】
本品主要成分为马发兰左旋体苯丙按酸氮芥
化学名:L-3{对[双(2-氯乙基)胺基]苯基}丙氨酸。
分子式:C13H18O2N2Cl2。
分子量:305.20克/摩尔。
【适应症/功能主治】
适用于治疗多发性骨髓瘤及晚期卵巢腺癌,在单一及联合化疗中是多发性骨髓瘤的首选药物。马法兰单独应用或与其他药物合用,对于部分晚期乳腺癌病人有显著疗效。
【规格型号】2mg片剂*25片
【用法用量】
因为马法兰具有骨髓抑制作用,故在治疗期间内,必需频繁监测血象(血细胞计数),必要时暂缓用药或调整剂量。成年口服用药:口服马发兰的吸收是易变的,为了确保达到可能的治疗水平。应谨慎增加剂量,直到出现出现骨髓抑制作用为止。
多发性骨髓瘤:
通常的口服剂量是每天6毫克(3片)。整个日剂量可以一次给予。根据每周进行的血细胞计数调整剂量。治疗2〜3周后,应停药4周,在此期间仔细观察血细胞计数。当白血球和血小板计数上升时,可以每天维持2毫克的剂量。由于口服药物后马发兰的血浆水平因人而异,几位研究者已经建议ALKERAN的剂量应谨慎得加量,直到观察到骨髓抑制,以确保药物的潜在治疗水平已经达到。其他剂量方案已由各种研究者使用。 Osserman和Takatsuki使用了每天10毫克/天,初始疗程7至10天。他们报告白细胞和血小板计数的最大抑制发生在3至5周内,并在4至8周内恢复。
当白细胞计数大于4,000个细胞/ mcL,血小板计数大于100,000个细胞/ mcL时,建立2mg /天的持续维持治疗。根据血液学反应,将剂量调整至1至3mg /天。希望保持显着程度的骨髓抑制,以保持白细胞计数在3,000至3,500细胞/ mcL的范围内。 Hoogstraten等人开始用0.15mg / kg /天进行治疗7天。其后休息至少14天,但可能长达5至6周。当白血球和血小板计数升高时开始维持治疗。维持剂量为0.05mg / kg /天或更少,并根据血液计数进行调整。有证据表明,大约三分之一到一半的多发性骨髓瘤患者对口服药物有良好的反应。
Alexanian等人的一项研究表明,ALKERAN与强的松组合的使用显着提高了多发性骨髓瘤患者达到缓解的百分比。一个方案是以0.25mg / kg /天连续连续4天(或连续5天为0.20mg / kg /天)施用ALKERAN疗程,总剂量为1mg / kg /疗程。如果粒细胞计数和血小板计数恢复正常水平,则每4至6周重复4至5天的疗程。要强调的是,反应可能在很多个月内是非常缓慢的;重要的是重复的疗程或连续治疗,因为改善可能会持续缓慢的多个月,如果治疗被放弃太早,可能会错过最大的好处。在中度至重度肾损伤的患者中,目前可获得的药代动力学数据不能证明对这些患者减少剂量的绝对推荐,但是最初使用降低剂量可能是谨慎的。 6参考编号:2940447
上皮性卵巢癌:一种常用的治疗卵巢癌的方案是以每日0.2mg / kg的剂量连用5天。 每4~8周或当外周血象恢复时重复疗程;当出现骨髓毒性时应减低剂量。
晚期乳腺癌:口服每日每公斤体重0.15毫克或每平方米体表面积6毫克,共5日,每六周重复疗程,也可使用美法仑静脉注射治疗。
真性红血球增多症:诱导缓解期,每日用6~10毫克共5~7天,之后可每日2~4毫克直至能满意地控制症状,维持剂量可每周一次用2~6毫克,其间必须对患者仔细谨慎地进行血液学控制,以血细胞计数结果为依据,适当调整剂量。
肾功能不全患者:依据目前建立的药动学数据,对中度至重度肾功能不全患者口服马法兰,并非绝对推荐降低剂量,但起始剂量需谨慎地降低。
【不良反应】
骨髓抑制:为剂量限制性毒性,主要表现为白细胞、血小板减少及贫血,白细胞减少可在首次用药后的第2周至第3周出现;有时老年患者骨髓抑制可延续5~6周
胃肠道反应:大剂量一次用药可出现恶心、呕吐,小剂量持续给药则不明显。
长期持续给药,偶可引起白血病、脱皮、皮炎、口炎及肺纤维化。
【禁忌】
孕妇、哺乳妇禁用。
近期内用过化疗或放疗而白细胞减少者不宜使用。
肾功能不良者慎用。
每次用药前须检查血像,嗜中性白细胞低于2×109/L时应停药。
应根据骨髓抑制程度调整剂量。
对此药过敏,请不要服用此药品;避免饮酒;避免服用Aspirin(Tapal)或感冒药,需告知医师;接受疫苗注射前,需告知医师;容易感染,需避免到公共场所及预防感冒等;不要哺乳、怀孕,接受此药后可能会造成不孕;易有口腔发炎、疮及刺刺的感觉,口腔清洁需撤底。若要预防恶心,呕吐,可请医师开立止吐药处方,医师可以会为病人抽血检查血象。
【孕妇及哺乳期妇女用药】
妊娠:有致畸作用。孕妇禁用
哺乳期妇女:不知道这种药物是否在人乳中排泄。 哺乳母亲禁用。
【儿童用药】
目前尚无用于儿童患者的安全性与疗效的资料。
【老年用药】
老年人用药安全性与有效性方面与年轻患者无显著差异。
【药理作用】
本品为左旋体苯丙氨酸氮芥,双氯乙胺型烷基化剂。是细胞周期非特异性药物。其细胞毒性与DNA的链间交联的程度有关,可能通过在鸟嘌呤的N7位置结合。像其他双功能烷基化剂一样,它对静止和迅速分裂的肿瘤细胞均具有作用。
口服吸收充分,服药后2小时血浆达到最浓度,在血浆中保持活性大约6小时,服药24小时内50%的药物经尿排泄,其中13%为原形,代谢产物为一羟衍生物及二羟衍生物。
【贮藏】
应在冰箱保存, 2° to 8°C (36° to 46°F). 避光.
文案整理: Dr. Jasmine Ding
PRESCRIBING INFORMATION
ALKERAN® (melphalan) Tablets
WARNING ALKERAN (melphalan) should be administered under the supervision of a qualified physician experienced in the use of cancer chemotherapeutic agents. Severe bone marrow suppression with resulting infection or bleeding may occur. Melphalan is leukemogenic in humans. Melphalan produces chromosomal aberrations in vitro and in vivo and, therefore, should be considered potentially mutagenic in humans.
DESCRIPTION
ALKERAN (melphalan), also known as L-phenylalanine mustard, phenylalanine mustard, L-PAM, or L-sarcolysin, is a phenylalanine derivative of nitrogen mustard. Melphalan is a bifunctional alkylating agent which is active against selective human neoplastic diseases. It is known chemically as 4-[bis(2-chloroethyl)amino]-L-phenylalanine. The molecular formula is C13H18Cl2N2O2 and the molecular weight is 305.20.
The structural formula is: Melphalan is the active L-isomer of the compound and was first synthesized in 1953 by Bergel and Stock; the D-isomer, known as medphalan, is less active against certain animal tumors, and the dose needed to produce effects on chromosomes is larger than that required with the L-isomer. The racemic (DL–) form is known as merphalan or sarcolysin. Melphalan is practically insoluble in water and has a pKa1 of ∼2.5.
ALKERAN (melphalan) is available in tablet form for oral administration. Each film-coated tablet contains 2 mg melphalan and the inactive ingredients colloidal silicon dioxide, crospovidone, hypromellose, macrogol/PEG 400, magnesium stearate, microcrystalline cellulose, and titanium dioxide.
CLINICAL PHARMACOLOGY
Melphalan is an alkylating agent of the bischloroethylamine type. As a result, its cytotoxicity appears to be related to the extent of its interstrand cross-linking with DNA, probably by binding at the N7 position of guanine. Like other bifunctional alkylating agents, it is active against both resting and rapidly dividing tumor cells.
Pharmacokinetics:
The pharmacokinetics of ALKERAN after oral administration has been 1 Reference ID: 2940447 extensively studied in adult patients. Plasma melphalan levels are highly variable after oral dosing, both with respect to the time of the first appearance of melphalan in plasma (range approximately 0 to 6 hours) and to the peak plasma concentration (Cmax) (range 70 to 4,000 ng/mL, depending upon the dose) achieved. These results may be due to incomplete intestinal absorption, a variable “first pass” hepatic metabolism, or to rapid hydrolysis. Five patients were studied after both oral and intravenous (IV) dosing with 0.6 mg/kg as a single bolus dose by each route. The areas under the plasma concentration-time curves (AUC) after oral administration averaged 61% ± 26% (± standard deviation [SD]; range 25% to 89%) of those following IV administration. In 18 patients given a single oral dose of 0.6 mg/kg of ALKERAN, the terminal elimination plasma half-life (t1/2) of parent drug was 1.5 ± 0.83 hours. The 24-hour urinary excretion of parent drug in these patients was 10% ± 4.5%, suggesting that renal clearance is not a major route of elimination of parent drug.
In a separate study in 18 patients given single oral doses of 0.2 to 0.25 mg/kg of ALKERAN, Cmax and AUC, when dose adjusted to a dose of 14 mg, were (mean ± SD) 212 ± 74 ng/mL and 498 ± 137 ng•hr/mL, respectively.
Elimination phase t½ in these patients was approximately 1 hour and the median tmax was 1 hour.
One study using universally labeled 14C-melphalan, found substantially less radioactivity in the urine of patients given the drug by mouth (30% of administered dose in 9 days) than in the urine of those given it intravenously (35% to 65% in 7 days). Following either oral or IV administration, the pattern of label recovery was similar, with the majority being recovered in the first 24 hours. Following oral administration, peak radioactivity occurred in plasma at 2 hours and then disappeared with a half-life of approximately 160 hours. In 1 patient where parent drug (rather than just radiolabel) was determined, the melphalan half-disappearance time was 67 minutes. The steady-state volume of distribution of melphalan is 0.5 L/kg. Penetration into cerebrospinal fluid (CSF) is low. The extent of melphalan binding to plasma proteins ranges from 60% to 90%. Serum albumin is the major binding protein, while α1-acid glycoprotein appears to account for about 20% of the plasma protein binding. Approximately 30% of melphalan is (covalently) irreversibly bound to plasma proteins. Interactions with immunoglobulins have been found to be negligible. Melphalan is eliminated from plasma primarily by chemical hydrolysis to monohydroxymelphalan and dihydroxymelphalan. Aside from these hydrolysis products, no other melphalan metabolites have been observed in humans. Although the contribution of renal elimination to melphalan clearance appears to be low, one pharmacokinetic study showed a significant positive correlation between the elimination rate constant for melphalan and renal function and a significant negative correlation between renal function and the area under the plasma melphalan concentration/time curve.
INDICATIONS AND USAGE
ALKERAN Tablets are indicated for the palliative treatment of multiple myeloma and for the palliation of non-resectable epithelial carcinoma of the ovary. Reference ID: 2940447
CONTRAINDICATIONS
ALKERAN should not be used in patients whose disease has demonstrated a prior resistance to this agent. Patients who have demonstrated hypersensitivity to melphalan should not be given the drug.
WARNINGS
ALKERAN should be administered in carefully adjusted dosage by or under the supervision of experienced physicians who are familiar with the drug's actions and the possible complications of its use. As with other nitrogen mustard drugs, excessive dosage will produce marked bone marrow suppression. Bone marrow suppression is the most significant toxicity associated with ALKERAN in most patients. Therefore, the following tests should be performed at the start of therapy and prior to each subsequent course of ALKERAN: platelet count, hemoglobin, white blood cell count, and differential. Thrombocytopenia and/or leukopenia are indications to withhold further therapy until the blood counts have sufficiently recovered. Frequent blood counts are essential to determine optimal dosage and to avoid toxicity (see PRECAUTIONS: Laboratory Tests). Dose adjustment on the basis of blood counts at the nadir and day of treatment should be considered. Hypersensitivity reactions, including anaphylaxis, have occurred rarely (see ADVERSE REACTIONS). These reactions have occurred after multiple courses of treatment and have recurred in patients who experienced a hypersensitivity reaction to IV ALKERAN. If a hypersensitivity reaction occurs, oral or IV ALKERAN should not be readministered.
Carcinogenesis: Secondary malignancies, including acute nonlymphocytic leukemia, myeloproliferative syndrome, and carcinoma have been reported in patients with cancer treated with alkylating agents (including melphalan). Some patients also received other chemotherapeutic agents or radiation therapy. Precise quantitation of the risk of acute leukemia, myeloproliferative syndrome, or carcinoma is not possible. Published reports of leukemia in patients who have received melphalan (and other alkylating agents) suggest that the risk of leukemogenesis increases with chronicity of treatment and with cumulative dose. In one study, the 10-year cumulative risk of developing acute leukemia or myeloproliferative syndrome after melphalan therapy was 19.5% for cumulative doses ranging from 730 mg to 9,652 mg. In this same study, as well as in an additional study, the 10-year cumulative risk of developing acute leukemia or myeloproliferative syndrome after melphalan therapy was less than 2% for cumulative doses under 600 mg. This does not mean that there is a cumulative dose below which there is no risk of the induction of secondary malignancy. The potential benefits from melphalan therapy must be weighed on an individual basis against the possible risk of the induction of a second malignancy. Adequate and well-controlled carcinogenicity studies have not been conducted in animals. However, i.p. administration of melphalan in rats (5.4 to 10.8 mg/m2 ) and in mice (2.25 to 4.5 mg/m2 ) 3 times per week for 6 months followed by 12 months post-dose observation produced peritoneal sarcoma and lung tumors, respectively. 3 Reference ID: 2940447
Mutagenesis: ALKERAN has been shown to cause chromatid or chromosome damage in humans. Intramuscular administration of ALKERAN at 6 and 60 mg/m2 produced structural aberrations of the chromatid and chromosomes in bone marrow cells of Wistar rats. Impairment of Fertility: ALKERAN causes suppression of ovarian function in premenopausal women, resulting in amenorrhea in a significant number of patients. Reversible and irreversible testicular suppression have also been reported. Pregnancy: Pregnancy Category D. ALKERAN may cause fetal harm when administered to a pregnant woman. Melphalan was embryolethal and teratogenic in rats following oral (6 to 18 mg/m2 /day for 10 days) and intraperitoneal (18 mg/m2 ) administration. Malformations resulting from melphalan included alterations of the brain (underdevelopment, deformation, meningocele, and encephalocele) and eye (anophthalmia and microphthalmos), reduction of the mandible and tail, as well as hepatocele (exomphaly).
There are no adequate and well-controlled studies in pregnant women. If this drug is used during pregnancy, or if the patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus. Women of childbearing potential should be advised to avoid becoming pregnant.
PRECAUTIONS
General:
In all instances where the use of ALKERAN is considered for chemotherapy, the physician must evaluate the need and usefulness of the drug against the risk of adverse events. ALKERAN should be used with extreme caution in patients whose bone marrow reserve may have been compromised by prior irradiation or chemotherapy, or whose marrow function is recovering from previous cytotoxic therapy. If the leukocyte count falls below 3,000 cells/mcL, or the platelet count below 100,000 cells/mcL, ALKERAN should be discontinued until the peripheral blood cell counts have recovered. A recommendation as to whether or not dosage reduction should be made routinely in patients with renal insufficiency cannot be made because: a) There is considerable inherent patient-to-patient variability in the systemic availability of melphalan in patients with normal renal function. b) Only a small amount of the administered dose appears as parent drug in the urine of patients with normal renal function. Patients with azotemia should be closely observed, however, in order to make dosage reductions, if required, at the earliest possible time. Administration of live vaccines to immunocompromised patients should be avoided.
for Patients: Patients should be informed that the major toxicities of ALKERAN are related to bone marrow suppression, hypersensitivity reactions, gastrointestinal toxicity, and pulmonary toxicity.
The major long-term toxicities are related to infertility and secondary malignancies. Patients should never be allowed to take the drug without close medical supervision and should be advised to consult their physician if they experience skin rash, vasculitis, bleeding, fever, persistent cough, nausea, vomiting, amenorrhea, weight loss, or 4 Reference ID: 2940447 unusual lumps/masses.
Women of childbearing potential should be advised to avoid becoming pregnant.
Laboratory Tests: Periodic complete blood counts with differentials should be performed during the course of treatment with ALKERAN. At least one determination should be obtained prior to each treatment course. Patients should be observed closely for consequences of bone marrow suppression, which include severe infections, bleeding, and symptomatic anemia (see WARNINGS). Drug Interactions: There are no known drug/drug interactions with oral ALKERAN.
Carcinogenesis, Mutagenesis, Impairment of Fertility:
See WARNINGS section.
Pregnancy: Teratogenic Effects: Pregnancy Category D: See WARNINGS section.
Nursing Mothers: It is not known whether this drug is excreted in human milk. ALKERAN should not be given to nursing mothers.
Pediatric Use: The safety and effectiveness of ALKERAN in pediatric patients have not been established.
Geriatric Use: Clinical studies of ALKERAN Tablets did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects. Other reported clinical experience has not identified differences in responses between the elderly and younger patients. In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy.
ADVERSE REACTIONS
Hematologic: The most common side effect is bone marrow suppression leading to leukopenia, thrombocytopenia, and anemia. Although bone marrow suppression frequently occurs, it is usually reversible if melphalan is withdrawn early enough. However, irreversible bone marrow failure has been reported. Gastrointestinal: Nausea, vomiting, diarrhea, and oral ulceration occur.
Hepatic disorders ranging from abnormal liver function tests to clinical manifestations such as hepatitis and jaundice have been reported.
Miscellaneous: Other reported adverse reactions include: pulmonary fibrosis (including fatal outcomes) and interstitial pneumonitis, skin hypersensitivity, maculopapular rashes, vasculitis, alopecia, and hemolytic anemia. Allergic reactions, including urticaria, edema, skin rashes, and rare anaphylaxis, have occurred after multiple courses of treatment.
Cardiac arrest has also been reported rarely in association with such reports.
OVERDOSAGE
Overdoses, including doses up to 50 mg/day for 16 days, have been reported. Immediate effects are likely to be vomiting, ulceration of the mouth, diarrhea, and hemorrhage of the gastrointestinal tract.
The principal toxic effect is bone marrow suppression. Hematologic parameters should be closely followed for 3 to 6 weeks. An uncontrolled study suggests that administration of autologous bone marrow or hematopoietic growth factors (i.e., sargramostim, 5 Reference ID: 2940447 filgrastim) may shorten the period of pancytopenia.
General supportive measures, together with appropriate blood transfusions and antibiotics, should be instituted as deemed necessary by the physician. This drug is not removed from plasma to any significant degree by hemodialysis.
DOSAGE AND ADMINISTRATION
Multiple Myeloma: The usual oral dose is 6 mg (3 tablets) daily. The entire daily dose may be given at one time. The dose is adjusted, as required, on the basis of blood counts done at approximately weekly intervals. After 2 to 3 weeks of treatment, the drug should be discontinued for up to 4 weeks, during which time the blood count should be followed carefully. When the white blood cell and platelet counts are rising, a maintenance dose of 2 mg daily may be instituted.
Because of the patient-to-patient variation in melphalan plasma levels following oral administration of the drug, several investigators have recommended that the dosage of ALKERAN be cautiously escalated until some myelosuppression is observed in order to assure that potentially therapeutic levels of the drug have been reached. Other dosage regimens have been used by various investigators. Osserman and Takatsuki have used an initial course of 10 mg/day for 7 to 10 days. They report that maximal suppression of the leukocyte and platelet counts occurs within 3 to 5 weeks and recovery within 4 to 8 weeks.
Continuous maintenance therapy with 2 mg/day is instituted when the white blood cell count is greater than 4,000 cells/mcL and the platelet count is greater than 100,000 cells/mcL. Dosage is adjusted to between 1 and 3 mg/day depending upon the hematological response. It is desirable to try to maintain a significant degree of bone marrow depression so as to keep the leukocyte count in the range of 3,000 to 3,500 cells/mcL. Hoogstraten et al have started treatment with 0.15 mg/kg/day for 7 days. This is followed by a rest period of at least 14 days, but it may be as long as 5 to 6 weeks. Maintenance therapy is started when the white blood cell and platelet counts are rising. The maintenance dose is 0.05 mg/kg/day or less and is adjusted according to the blood count. Available evidence suggests that about one third to one half of the patients with multiple myeloma show a favorable response to oral administration of the drug.
One study by Alexanian et al has shown that the use of ALKERAN in combination with prednisone significantly improves the percentage of patients with multiple myeloma who achieve palliation. One regimen has been to administer courses of ALKERAN at 0.25 mg/kg/day for 4 consecutive days (or, 0.20 mg/kg/day for 5 consecutive days) for a total dose of 1 mg/kg/course. These 4- to 5-day courses are then repeated every 4 to 6 weeks if the granulocyte count and the platelet count have returned to normal levels. It is to be emphasized that response may be very gradual over many months; it is important that repeated courses or continuous therapy be given since improvement may continue slowly over many months, and the maximum benefit may be missed if treatment is abandoned too soon. In patients with moderate to severe renal impairment, currently available pharmacokinetic data do not justify an absolute recommendation on dosage reduction to those patients, but it may be prudent to use a reduced dose initially. 6 Reference ID: 2940447
Epithelial Ovarian Cancer: One commonly employed regimen for the treatment of ovarian carcinoma has been to administer ALKERAN at a dose of 0.2 mg/kg daily for 5 days as a single course. Courses are repeated every 4 to 5 weeks depending upon hematologic tolerance. Administration Precautions: Procedures for proper handling and disposal of anticancer drugs should be considered. Several guidelines on this subject have been published.1-8 There is no general agreement that all of the procedures recommended in the guidelines are necessary or appropriate.
HOW SUPPLIED
ALKERAN is supplied as white, film-coated, round, biconvex tablets containing 2 mg melphalan in amber glass bottles with child-resistant closures. One side is engraved with “GX EH3” and the other side is engraved with an “A.” Bottle of 50 (NDC 59572-302-50).
Store in a refrigerator, 2° to 8°C (36° to 46°F). Protect from light.
REFERENCES
1. ONS Clinical Practice Committee. Cancer Chemotherapy Guidelines and Recommendations for Practice. Pittsburgh, PA: Oncology Nursing Society;1999:32-41.
2. Recommendations for the safe handling of parenteral antineoplastic drugs. Washington, DC: Division of Safety, Clinical Center Pharmacy Department and Cancer Nursing Services, National Institutes of Health; 1992. US Dept of Health and Human Services. Public Health Service publication NIH 92-2621.
3. AMA Council on Scientific Affairs. Guidelines for handling parenteral antineoplastics. JAMA. 1985;253:1590-1591. 4. National Study Commission on Cytotoxic Exposure. Recommendations for handling cytotoxic agents. 1987. Available from Louis P. Jeffrey, Chairman, National Study Commission on Cytotoxic Exposure. Massachusetts College of Pharmacy and Allied Health Sciences, 179 Longwood Avenue, Boston, MA 02115.
5. Clinical Oncological Society of Australia. Guidelines and recommendations for safe handling of antineoplastic agents. Med J Australia. 1983;1:426-428.
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