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轮状病毒VP4在体内的切割

Cleavage of rotavirus VP4 in vivo.

作者信息

Ludert J E, Krishnaney A A, Burns J W, Vo P T, Greenberg H B

机构信息

Division of Gastroenterology, Stanford University Medical School, California 94305, USA.

出版信息

J Gen Virol. 1996 Mar;77 ( Pt 3):391-5. doi: 10.1099/0022-1317-77-3-391.

Abstract

The infectivity of rotavirus particles is dependent on proteolytic cleavage of the outer capsid protein, VP4, at a specific site. This cleavage event yields two fragments, identified as VP5* and VP8*. It has been hypothesized that the particle is more stable, but non-infectious, when VP4 is in the uncleaved state. Uncleaved VP4 and the resultant increased stability might be advantageous for the virus to resist environmental degradation until it infects a susceptible host. When VP4 is cleaved in the lumen of the host's gastrointestinal tract, the virus particle would become less stable but more infectious. To test this hypothesis, a series of experiments was undertaken to analyse the cleavage state of VP4 on virus shed by an infected host into the environment. Immunoblots of intestinal wash solutions derived from infant and adult BALB/c mice infected with a virulent cell culture-adapted variant of the EDIM virus (EW) or wild-type murine rotavirus EDIM-Cambridge were analysed. Virtually all of the VP4 in these samples was in the cleaved form. Moreover, cell culture titration of trypsin-treated and untreated intestinal contents from pups infected with EW indicated that excreted virus is fully activated prior to trypsin addition. It was also observed that trypsin-activated virus has no disadvantage in initiating infection in naive animals over virions containing an intact VP4. These studies indicate that VP4 is cleaved upon release from the intestinal cell and that virus shed into the environment does not have an intact VP4.

摘要

轮状病毒颗粒的感染性取决于外衣壳蛋白VP4在特定位点的蛋白水解切割。这一切割事件产生两个片段,分别鉴定为VP5和VP8。据推测,当VP4处于未切割状态时,病毒颗粒更稳定但无感染性。未切割的VP4以及由此产生的更高稳定性可能有利于病毒抵抗环境降解,直到它感染易感宿主。当VP4在宿主胃肠道腔内被切割时,病毒颗粒会变得不太稳定但感染性更强。为了验证这一假设,进行了一系列实验来分析受感染宿主释放到环境中的病毒上VP4的切割状态。对感染了EDIM病毒(EW)的细胞培养适应性强毒株或野生型鼠轮状病毒EDIM-剑桥的幼鼠和成年BALB/c小鼠的肠道冲洗液进行免疫印迹分析。这些样本中几乎所有的VP4都处于切割形式。此外,对感染EW的幼崽的胰蛋白酶处理和未处理的肠道内容物进行细胞培养滴定表明,在添加胰蛋白酶之前,排出的病毒已被完全激活。还观察到,与含有完整VP4的病毒粒子相比,胰蛋白酶激活的病毒在感染未接触过该病毒的动物时没有劣势。这些研究表明,VP4在从肠道细胞释放时被切割,释放到环境中的病毒不具有完整的VP4。

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