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HIV-1病毒感染因子(vif)基因的体内遗传变异性

In vivo genetic variability of the HIV-1 vif gene.

作者信息

Wieland U, Hartmann J, Suhr H, Salzberger B, Eggers H J, Kühn J E

机构信息

Institut für Virologie, Universität zu Köln, Germany.

出版信息

Virology. 1994 Aug 15;203(1):43-51. doi: 10.1006/viro.1994.1453.

Abstract

The human immunodeficiency virus type 1 (HIV-1) vif gene encodes a 23-kDa protein (viral infectivity factor) whose exact mechanism of action is not entirely clear. Vif is believed to be highly conserved among different HIV-1 strains. We have analyzed the proviral vif sequences of 61 peripheral blood mononuclear cell samples from HIV-1 positive patients by direct solid phase sequencing and temperature gradient gel electrophoresis of polymerase chain reaction products. Inter- and intraindividual sequence variations, conserved motifs, and prevalent vif subtypes were investigated. The consensus proviral vif DNA sequence of the 61 samples as well as the consensus sequence of the 61 deduced vif amino acid sequences were found to be less conserved than previously thought. The vif proviral sequences were 58% conserved, with the 5' end of the vif gene being the most conserved region (84%). Of the vif amino acids only 45% were absolutely conserved in the 61 samples, i.e., the absolutely conserved and as such possibly functionally important domains of the vif protein comprised less than half of the vif amino acids. In two-thirds of the variable positions residues belonging to different amino acid groups were found. In individual patients the prevalent vif sequence changed with the course of disease, but the differences found in two serial samples of a patient were < or = 10%. Phylogenetic analysis revealed that one African vif subtype had been introduced in the investigated population.

摘要

人类免疫缺陷病毒1型(HIV-1)的vif基因编码一种23 kDa的蛋白质(病毒感染性因子),其确切作用机制尚不完全清楚。Vif被认为在不同的HIV-1毒株中高度保守。我们通过对聚合酶链反应产物进行直接固相测序和温度梯度凝胶电泳,分析了61例HIV-1阳性患者外周血单个核细胞样本的前病毒vif序列。研究了个体间和个体内的序列变异、保守基序以及流行的vif亚型。结果发现,61个样本的前病毒vif DNA共有序列以及61个推导的vif氨基酸序列的共有序列的保守性低于先前的认识。vif前病毒序列的保守性为58%,其中vif基因的5'端是最保守的区域(84%)。在61个样本中,vif氨基酸只有45%是绝对保守的,即vif蛋白中绝对保守且可能具有功能重要性的结构域不到vif氨基酸的一半。在三分之二的可变位点发现了属于不同氨基酸组的残基。在个体患者中,流行的vif序列随病程变化,但同一患者两个连续样本中的差异≤10%。系统发育分析显示,一种非洲vif亚型已引入所研究的人群。

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