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在人类免疫缺陷病毒1型不同基因谱系中观察到的V3环蛋白序列的突变趋势。

Mutational trends in V3 loop protein sequences observed in different genetic lineages of human immunodeficiency virus type 1.

作者信息

Korber B T, MacInnes K, Smith R F, Myers G

机构信息

Theoretical Division, Los Alamos National Laboratory, New Mexico 87545.

出版信息

J Virol. 1994 Oct;68(10):6730-44. doi: 10.1128/JVI.68.10.6730-6744.1994.

Abstract

Highly variable international human immunodeficiency virus type 1 envelope sequences can be assigned to six major clades, or phylogenetically defined subtypes, designated A through F. These subtypes are approximately equidistant in terms of evolutionary distance measured by nucleotide sequences. This radiation from a common ancestral sequence may have been in step with the spread of the pandemic. In this study, V3 loop protein sequence relationships within these major clades are analyzed to determine how the different lineages might be evolving with respect to this biologically important domain. The V3 loop has been shown to influence viral phenotype and to elicit both humoral and cellular immune responses. To identify patterns in V3 loop amino acid evolution, we cluster the sequences by a phenetic principle which evaluates protein similarities on the basis of amino acid identities and similarities irrespective of evolutionary relationships. When phenetic clustering patterns are superimposed upon phylogenetic subtype classifications, two interesting mutational trends are revealed. First, a set of identical, or highly similar, V3 loop protein sequences can be identified within two otherwise dissimilar genetic subtypes, A and C. Second, the D subtype sequences are found to possess the most radically divergent set of V3 loop sequences. These and other patterns characteristic of the V3 loop reflect the acquisition of specific biological properties during the apparently recent evolution of the human immunodeficiency virus type 1 lineages.

摘要

高度可变的国际1型人类免疫缺陷病毒包膜序列可被归为六个主要分支,即系统发育定义的亚型,命名为A至F。就核苷酸序列测量的进化距离而言,这些亚型大致等距。从共同祖先序列的这种辐射可能与大流行的传播同步。在本研究中,分析了这些主要分支内的V3环蛋白序列关系,以确定不同谱系在这个生物学上重要的结构域方面可能如何进化。V3环已被证明会影响病毒表型,并引发体液免疫和细胞免疫反应。为了识别V3环氨基酸进化中的模式,我们根据一种表型原则对序列进行聚类,该原则基于氨基酸同一性和相似性评估蛋白质相似性,而不考虑进化关系。当将表型聚类模式叠加到系统发育亚型分类上时,揭示了两个有趣的突变趋势。首先,在另外两个不同的基因亚型A和C中,可以鉴定出一组相同或高度相似的V3环蛋白序列。其次,发现D亚型序列拥有最具根本性差异的V3环序列集。V3环的这些以及其他特征模式反映了在1型人类免疫缺陷病毒谱系最近的进化过程中特定生物学特性的获得。

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