Virus-specific cytotoxic T-lymphocyte responses select for amino-acid variation in simian immunodeficiency virus Env and Nef

被引:0
作者
David T. Evans
David H. O'Connor
Peicheng Jing
John L. Dzuris
John Sidney
Jack da Silva
Todd M. Allen
Helen Horton
John E. Venham
Richard A. Rudersdorf
Thorsten Vogel
C. David Pauza
Ronald E. Bontrop
Robert DeMars
Alessandro Sette
Austin L. Hughes
David I. Watkins
机构
[1] Wisconsin Regional Primate Research Center,Department of Pathology and Laboratory Medicine
[2] University of Wisconsin,New England Regional Primate Research Center
[3] Epimmune,Department of Biology
[4] Institute of Molecular Evolutionary Genetics,undefined
[5] The Pennsylvania State University,undefined
[6] Laboratory of Genetics,undefined
[7] Genetics Building,undefined
[8] University of Wisconsin,undefined
[9] University of Wisconsin,undefined
[10] Biomedical Primate Research Centre-TNO,undefined
[11] Harvard Medical School,undefined
[12] One Pine Hill Drive,undefined
[13] East Carolina University,undefined
来源
Nature Medicine | 1999年 / 5卷
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摘要
Cytotoxic T-lymphocyte (CTL) responses to human immunodeficiency virus arise early after infection, but ultimately fail to prevent progression to AIDS. Human immunodeficiency virus may evade the CTL response by accumulating amino-acid replacements within CTL epitopes. We studied 10 CTL epitopes during the course of simian immunodeficiency virus disease progression in three related macaques. All 10 of these CTL epitopes accumulated amino-acid replacements and showed evidence of positive selection by the time the macaques died. Many of the amino-acid replacements in these epitopes reduced or eliminated major histocompatibility complex class I binding and/or CTL recognition. These findings strongly support the CTL 'escape' hypothesis.
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页码:1270 / 1276
页数:6
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