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人类和黑猩猩免疫缺陷病毒中的正向选择与进化速率

Positive selection and rates of evolution in immunodeficiency viruses from humans and chimpanzees.

作者信息

Mindell D P

机构信息

Department of Biology and Museum of Zoology, University of Michigan, Ann Arbor, MI 48109, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Apr 16;93(8):3284-8. doi: 10.1073/pnas.93.8.3284.

DOI:10.1073/pnas.93.8.3284
PMID:8622929
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC39598/
Abstract

Evolutionary theory predicts the recent spread of primate immunodeficiency viruses (PIVs) to new human populations to be accompanied by positive selection in response to new host environments and/or by random genetic drift. I assess evidence for positive selection in human and chimpanzee PIVs type I (PIV1s), using ratios of synonymous to nonsynonymous nucleotide change based on branch lengths and outgroup rooting. Ratios are smaller for PIV1s from humans than for PIV1 from a chimpanzee for the pol, gag, and env glycoprotein 120 (gp120) regions, indicating greater effects of positive selection in PIV1s from humans. Parsimony-based relative rate tests for amino acid changes showed significant differences between PIV1s from humans and chimpanzees in 18 of 48 pairwise comparisons, with all 18 showing faster rates of change in PIV1s from humans. This study indicates that in some instances, the recent evolution of human PIV1s follows a speciational pattern, in which increased diversification of taxa is correlated with greater amounts of character change appearing and being maintained through time. This extends the generality of the speciational pattern to a group of organisms (viruses) having the fastest known rates of anagenetic change for nucleotide characters and indicates that comprehensive understanding of PIV1 evolution requires consideration of both anagenetic change within viral lineages and the relative historical success of different viral clades. Phylogenetic analyses show that neither PIV1s infecting humans nor those infecting chimpanzees represent monophyletic groups and suggest multiple host-species shifts for PIV1s.

摘要

进化理论预测,灵长类免疫缺陷病毒(PIVs)近期向新的人类群体传播时,会伴随着因应新宿主环境的正选择和/或随机遗传漂变。我基于分支长度和外类群生根,使用同义核苷酸变化与非同义核苷酸变化的比率,评估人类和黑猩猩I型PIVs(PIV1s)中正向选择的证据。对于来自人类的PIV1s,其在pol、gag和包膜糖蛋白120(gp120)区域的比率低于来自黑猩猩的PIV1,这表明来自人类的PIV1s中正向选择的影响更大。基于简约法的氨基酸变化相对速率测试显示,在48对比较中的18对中,人类和黑猩猩的PIV1s之间存在显著差异,所有18对都显示人类PIV1s的变化速率更快。这项研究表明,在某些情况下,人类PIV1s的近期进化遵循一种物种形成模式,即分类群的多样化增加与随时间出现并维持的更多性状变化相关。这将物种形成模式的普遍性扩展到了一组具有已知最快核苷酸性状前进演化变化速率的生物体(病毒),并表明对PIV1进化的全面理解需要考虑病毒谱系内的前进演化变化以及不同病毒分支的相对历史成功情况。系统发育分析表明,感染人类的PIV1s和感染黑猩猩的PIV1s都不代表单系群,并表明PIV1s存在多次宿主物种转移。