HIV infection induces changes in CD4+ T-cell phenotype and depletions within the CD4+ T-cell repertoire that are not immediately restored by antiviral or immune-based therapies

被引:0
|
作者
Mark Connors
Joseph A. Kovacs
Seth Krevat
Juan C. Gea-Banacloche
Michael C. Sneller
Mark Flanigan
Julia A. Metcalf
Robert E. Walker
Judith Falloon
Michael Baseler
Randy Stevens
Irwin Feuerstein
Henry Masur
H. Clifford Lane
机构
[1] National Institutes of Health,Laboratory of lmmunoregulation of the National Institute of Allergy and Infectious Diseases
[2] National Institutes of Health,Clinical Center, Critical Care Medicine Department
[3] Servicio de Medicina Intema 1,Frederick Cancer Research and Development Center, Science Application International Corporation
[4] Clinica Puerta de Hierreo,Clinical Center, Diagnostic Radiology
[5] National Cancer Institute,undefined
[6] National Institutes of Health,undefined
来源
Nature Medicine | 1997年 / 3卷
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摘要
Changes in CD4+ T-cell surface marker phenotype and antigen receptor (TCR) repertoire were examined during the course of HIV infection and following therapy. A preferential decline in naive CD4+ T cells was noted as disease progressed. Following protease inhibitor therapy, naive CD4+ T cells increased only if they were present before initiation of therapy. Disruptions of the CD4+ TCR repertoire were most prevalent in patients with the lowest CD4+ T-cell counts. Antiviral or IL-12 therapy-induced increases in CD4+ T-cell counts led to only minor changes in previously disrupted repertoires. Thus, CD4+ T-cell death mediated by HIV-1 infection may result in a preferential decline in the number of naive CD4+ T cells and disruptions of the CD4+T-cell repertoire that are not immediately corrected by antiviral or immune-based therapies.
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页码:533 / 540
页数:7
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