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人γ干扰素的分解代谢部位

Catabolic sites of human interferon-gamma.

作者信息

Bocci V, Pacini A, Pessina G P, Paulesu L, Muscettola M, Lunghetti G

出版信息

J Gen Virol. 1985 Apr;66 ( Pt 4):887-91. doi: 10.1099/0022-1317-66-4-887.

Abstract

Recombinant human interferon-gamma (HuIFN-gamma) injected into rabbits disappeared from the circulation more rapidly than natural IFN-gamma. The latter displayed an initial decay curve more rapid than that for natural HuIFN-alpha although 4 h after injection plasma levels were similar. This result suggests that IFN-gamma has pharmacokinetic properties different to those of IFN-alpha which may be explained by considerable and simultaneous hepatic and renal catabolism. Surprisingly, the hepatic uptake of recombinant (unglycosylated) IFN-gamma was more marked than uptake of natural IFN-gamma. Moreover, both IFN-gamma preparations were cleared by the isolated and perfused kidney and once again the recombinant IFN disappeared more rapidly. This result does not conform with the suggestion that IFN-gamma exists as a tetramer which would not be filtered by the glomerulus, but is consistent with the pharmacokinetic behaviour shown in vivo.

摘要

注入兔子体内的重组人干扰素-γ(HuIFN-γ)从循环系统中消失的速度比天然干扰素-γ更快。尽管注射后4小时血浆水平相似,但天然干扰素-γ的初始衰减曲线比天然HuIFN-α的更快。这一结果表明,干扰素-γ具有与干扰素-α不同的药代动力学特性,这可能是由于肝脏和肾脏同时进行的大量分解代谢所致。令人惊讶的是,重组(未糖基化)干扰素-γ的肝脏摄取比天然干扰素-γ更显著。此外,两种干扰素-γ制剂都能被分离并灌注的肾脏清除,重组干扰素再次更快地消失。这一结果与干扰素-γ以四聚体形式存在因而不会被肾小球滤过的观点不符,但与体内显示的药代动力学行为一致。

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