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通过暴露于磷酸三(正丁基)酯和胆酸钠对肝炎病毒和人嗜T淋巴细胞病毒III型进行灭活

Sterilisation of hepatitis and HTLV-III viruses by exposure to tri(n-butyl)phosphate and sodium cholate.

作者信息

Prince A M, Horowitz B, Brotman B

出版信息

Lancet. 1986 Mar 29;1(8483):706-10. doi: 10.1016/s0140-6736(86)91101-3.

Abstract

Blood product sterilisation with 0.3% tri(n-butyl)phosphate (TNBP)/0.2% sodium cholate (CA), a combination known to permit high recovery of factor VIII and factor IX, was evaluated for its effect on hepatitis B (HBV), non-A, non-B (NANB), and human T-lymphotropic type III (HTLV-III) viruses. 2 chimpanzees received factor VIII preparations contaminated with 10(4) chimpanzee infectious doses (CID50) of HBV and treated with TNBP/CA; neither had evidence of HBV infection during 9 months follow-up, but hepatitis B surface antigen (HBsAg) developed 5 and 6 weeks, respectively, after challenge with untreated inoculum. 2 chimpanzees were similarly exposed to 10(4) CID50 of Hutchinson NANB inoculum treated with TNBP/CA; neither became infected during 26 weeks of follow-up but both had characteristic NANB-associated ultrastructural changes 3-5 weeks after exposure to untreated inoculum. 2 chimpanzees inoculated with 80 ml of TNBP/CA-treated factor VIII derived from a pool of thirteen lots obtained from five US manufacturers remained free of any evidence of NANB infection during 32 weeks of follow-up. Subsequently, NANB infection developed in both animals 3-4 weeks after exposure to untreated inoculum. Exposure of HTLV-III diluted into a factor VIII preparation to TNBP/CA inactivated greater than or equal to 10(4.2) tissue culture infective doses within 20 min at 24 degrees C.

摘要

用0.3%磷酸三(正丁基)酯(TNBP)/0.2%胆酸钠(CA)对血液制品进行消毒,已知该组合能使凝血因子VIII和凝血因子IX有较高回收率,对其对乙型肝炎病毒(HBV)、非甲非乙型肝炎病毒(NANB)和人类嗜T淋巴细胞病毒III型(HTLV-III)的影响进行了评估。2只黑猩猩接受了被10⁴黑猩猩感染剂量(CID50)的HBV污染并用TNBP/CA处理的凝血因子VIII制剂;在9个月的随访期间,两只黑猩猩均无HBV感染的证据,但在用未处理的接种物攻击后分别在5周和6周出现了乙型肝炎表面抗原(HBsAg)。2只黑猩猩同样暴露于用TNBP/CA处理的10⁴CID50的哈钦森NANB接种物;在26周的随访期间,两只黑猩猩均未感染,但在暴露于未处理的接种物后3 - 5周,两只黑猩猩均出现了与NANB相关的特征性超微结构变化。2只黑猩猩接种了从5家美国制造商获得的13批混合而成的经TNBP/CA处理的凝血因子VIII 80毫升,在32周的随访期间均未出现任何NANB感染的证据。随后,两只动物在暴露于未处理的接种物后3 - 4周均发生了NANB感染。将稀释到凝血因子VIII制剂中的HTLV-III在24℃下用TNBP/CA处理20分钟内可灭活≥10⁴·²组织培养感染剂量。

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