作者
Christof Geldmacher, Njabulo Ngwenyama, Alexandra Schuetz, Constantinos Petrovas, Klaus Reither, Edwin J Heeregrave, Joseph P Casazza, David R Ambrozak, Mark Louder, William Ampofo, Georgios Pollakis, Brenna Hill, Erica Sanga, Elmar Saathoff, Leonard Maboko, Mario Roederer, William A Paxton, Michael Hoelscher, Richard A Koup
发表日期
2010/12/20
期刊
Journal of Experimental Medicine
卷号
207
期号
13
页码范围
2869-2881
出版商
The Rockefeller University Press
简介
HIV-1 infection results in the progressive loss of CD4 T cells. In this study, we address how different pathogen-specific CD4 T cells are affected by HIV infection and the cellular parameters involved. We found striking differences in the depletion rates between CD4 T cells to two common opportunistic pathogens, cytomegalovirus (CMV) and Mycobacterium tuberculosis (MTB). CMV-specific CD4 T cells persisted after HIV infection, whereas MTB-specific CD4 T cells were depleted rapidly. CMV-specific CD4 T cells expressed a mature phenotype and produced very little IL-2, but large amounts of MIP-1β. In contrast, MTB-specific CD4 T cells were less mature, and most produced IL-2 but not MIP-1β. Staphylococcal enterotoxin B–stimulated IL-2–producing cells were more susceptible to HIV infection in vitro than MIP-1β–producing cells. Moreover, IL-2 production was associated with expression of CD25, and …
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