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用于持续输注的单克隆纯化因子VIII:稳定性、微生物安全性及临床经验

Monoclonal purified F VIII for continuous infusion: stability, microbiological safety and clinical experience.

作者信息

Schulman S, Varon D, Keller N, Gitel S, Martinowitz U

机构信息

National Hemophilia Center, Chaim Sheba Medical Center, Tel-Hashomer, Israel.

出版信息

Thromb Haemost. 1994 Sep;72(3):403-7.

PMID:7855792
Abstract

Replacement therapy for patients with hemophilia A postoperatively or for major hemorrhage, administered as a continuous infusion, is efficient and reduces the requirement for factor VIII (F VIII). The convenience of the method is increased by using a minipump and not diluting the concentrate further after reconstitution. A monoclonally purified F VIII concentrate (Monoclate-P), was evaluated for its stability after reconstitution in different infusion systems, for its microbiological safety as well as clinical safety and efficacy in continuous infusion. The F VIII activity was unaffected by 2 of the 3 infusion systems at room temperature during 15 days, whereas in the third (CADD-1) it decreased below 80% of initial value after 3-7 days. Addition of heparin (1 U/ml) or low molecular weight heparin (1 anti-Xa U/ml), which are used to prevent thrombophlebitis at the site of infusion, did not affect the stability. Nine out of 9 samples taken from the infusion systems after 3 days and again after 7 days were sterile. After inoculation with Staphylococcus aureus or Escherichia coli the bacterial growth in samples of the reconstituted concentrate was not different from that in lidocaine in saline or heparin in saline. F VIII was given in continuous infusion with a minipump (Infu-Med) to 12 patients undergoing major surgery and 8 patients with major hemorrhage for a total of 157 days. A progressive decrease of the clearance was seen during the first 5 days of infusion from 3.0 to 1.7 ml/kg/h. Hemostasis was effectively achieved, and no infectious complications were registered.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对于甲型血友病患者术后或大出血时,采用持续输注进行替代治疗是有效的,且可减少对凝血因子VIII(F VIII)的需求。使用微型泵并在复溶后不再进一步稀释浓缩物,增加了该方法的便利性。对一种单克隆纯化的F VIII浓缩物(Monoclate-P)在不同输注系统中复溶后的稳定性、微生物安全性以及持续输注时的临床安全性和有效性进行了评估。在室温下,15天内3种输注系统中的2种对F VIII活性无影响,而在第三种(CADD-1)系统中,3 - 7天后其活性降至初始值的80%以下。添加用于预防输注部位血栓性静脉炎的肝素(1 U/ml)或低分子量肝素(1抗Xa U/ml)不影响稳定性。3天后和7天后从输注系统中采集的9个样本中有9个无菌。用金黄色葡萄球菌或大肠杆菌接种后,复溶浓缩物样本中的细菌生长与盐水中利多卡因或盐水中肝素的样本无差异。使用微型泵(Infu-Med)对12例接受大手术的患者和8例大出血患者进行F VIII持续输注,共157天。输注的前5天内清除率逐渐下降,从3.0降至1.7 ml/kg/h。有效实现了止血,且未记录到感染并发症。(摘要截短于250字)

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