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病毒持续存在的遗传基础:病毒糖蛋白中的单个氨基酸变化影响淋巴细胞性脉络丛脑膜炎病毒在成年小鼠体内持续存在的能力。

Genetic basis of viral persistence: single amino acid change in the viral glycoprotein affects ability of lymphocytic choriomeningitis virus to persist in adult mice.

作者信息

Matloubian M, Somasundaram T, Kolhekar S R, Selvakumar R, Ahmed R

机构信息

Department of Microbiology and Immunology, UCLA School of Medicine 90024.

出版信息

J Exp Med. 1990 Oct 1;172(4):1043-8. doi: 10.1084/jem.172.4.1043.

Abstract

This study has identified a single amino acid change in the viral glycoprotein that profoundly affects the ability of lymphocytic choriomeningitis virus (LCMV) to persist in its natural host. Adult immunocompetent mice infected with a variant of the Armstrong strain, spleen isolate clone 13 (svA/svA), harbor virus for several months and exhibit suppressed T cell responses. In contrast, adult mice infected with a reassortant virus (svA/wtA) that contains the L segment of the spleen variant and the S segment of the parental wt Armstrong, make potent LCMV-specific CTL responses and clear the infection within 2-4 wk. These two viruses, spleen variant clone 13 and the reassortant svA/wtA, are identical in their noncoding regions and show no amino acid changes in any of their viral genes except for one substitution in the glycoprotein. The reassortant virus svA/wtA has a phenylalanine at amino acid residue 260 of the glycoprotein, whereas the spleen variant clone 13 has a leucine at this position. This study constitutes one of the first reports defining the genetic basis of viral persistence at the whole animal level, and identifying a single mutation that markedly increases the ability of a virus to persist in its natural host.

摘要

本研究确定了病毒糖蛋白中的一个单氨基酸变化,该变化深刻影响淋巴细胞性脉络丛脑膜炎病毒(LCMV)在其天然宿主中持续存在的能力。用阿姆斯特朗毒株的一个变体——脾脏分离株克隆13(svA/svA)感染成年免疫活性小鼠,病毒可在其体内存留数月,且T细胞反应受到抑制。相比之下,用一种重配病毒(svA/wtA)感染成年小鼠,该病毒含有脾脏变体的L片段和亲本野生型阿姆斯特朗的S片段,小鼠会产生有效的LCMV特异性CTL反应,并在2至4周内清除感染。这两种病毒,即脾脏变体克隆13和重配病毒svA/wtA,在非编码区相同,除糖蛋白中有一个氨基酸替换外,其任何病毒基因均无氨基酸变化。重配病毒svA/wtA在糖蛋白的氨基酸残基260处为苯丙氨酸,而脾脏变体克隆13在该位置为亮氨酸。本研究是最早在全动物水平定义病毒持续存在的遗传基础,并确定一个显著增加病毒在其天然宿主中持续存在能力的单一突变的报告之一。

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