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通过对人凝血因子VIII浓缩物进行热处理降低肝炎传播风险。

Reduction in risk of hepatitis transmission by heat-treatment of a human Factor VIII concentrate.

作者信息

Hollinger F B, Dolana G, Thomas W, Gyorkey F

出版信息

J Infect Dis. 1984 Aug;150(2):250-62. doi: 10.1093/infdis/150.2.250.

Abstract

A human Factor VIII concentrate containing both a non-A, non-B hepatitis agent and 300 or 30,000 chimpanzee infectious doses of added hepatitis B virus (HBV) was heated to 60 C in the lyophilized state for more than 10 hr. None of the four test chimpanzees that received the heated concentrate developed biochemical or ultrastructural evidence of non-A, non-B hepatitis, whereas both control animals receiving unheated product acquired the disease four to five weeks after infusion. In one of these animals the alanine aminotransferase level remained elevated, a finding indicating unresolved or persistent liver disease. Challenge inoculations with unheated Factor VIII base product (without HBV) resulted in the development of non-A, non-B hepatitis in one of two chimpanzees that previously received the heated product. Hepatitis B infection developed in the control animal that resolved its non-A, non-B hepatitis infection but not in the non-A, non-B hepatitis carrier chimpanzee. Both chimpanzees receiving the heated Factor VIII containing 300 chimpanzee infectious doses of HBV failed to develop hepatitis B until 32 and 40 weeks postinoculation, whereas the two chimpanzees that received heated concentrate containing 30,000 infectious doses of HBV became infected within the expected time. Product characterization and human safety trials have revealed no significant difference between the heated and unheated Factor VIII lots and recovery of product has been exceptionally good.

摘要

一种含有非甲非乙型肝炎病原体以及300或30000个黑猩猩感染剂量的添加乙型肝炎病毒(HBV)的人凝血因子VIII浓缩物,在冻干状态下加热至60℃超过10小时。接受加热浓缩物的四只试验黑猩猩均未出现非甲非乙型肝炎的生化或超微结构证据,而接受未加热产品的两只对照动物在输注后四到五周患上了该病。在其中一只动物中,丙氨酸转氨酶水平持续升高,这一发现表明存在未解决的或持续性肝病。用未加热的凝血因子VIII基础产品(不含HBV)进行激发接种,导致两只先前接受加热产品的黑猩猩中的一只患上了非甲非乙型肝炎。在解决了非甲非乙型肝炎感染的对照动物中发生了乙型肝炎感染,但在非甲非乙型肝炎携带黑猩猩中未发生。接受含有300个黑猩猩感染剂量HBV的加热凝血因子VIII的两只黑猩猩,直到接种后32周和40周才出现乙型肝炎,而接受含有30000个感染剂量HBV的加热浓缩物的两只黑猩猩在预期时间内被感染。产品特性分析和人体安全性试验表明,加热和未加热的凝血因子VIII批次之间没有显著差异,并且产品回收率非常高。

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