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HIV-1感染中持续的免疫激活与发展为艾滋病相关。

Persistent immune activation in HIV-1 infection is associated with progression to AIDS.

作者信息

Hazenberg Mette D, Otto Sigrid A, van Benthem Birgit H B, Roos Marijke Th L, Coutinho Roel A, Lange Joep M A, Hamann Dörte, Prins Maria, Miedema Frank

机构信息

Department of Clinical Viro-Immunology, Sanquin Research at CLB, Tropical Medicine and AIDS, Amsterdam, The Netherlands.

出版信息

AIDS. 2003 Sep 5;17(13):1881-8. doi: 10.1097/00002030-200309050-00006.

DOI:10.1097/00002030-200309050-00006
PMID:12960820
Abstract

BACKGROUND

HIV-1 infection is characterized by chronic generalized CD8 and CD4 T cell hyperactivation, the biological effect of which is not understood.

OBJECTIVE

To study the relation between chronic immune activation and CD4 T cell depletion in HIV-1 infection.

DESIGN

Prospective cohort study among participants of the Amsterdam Cohort Studies on HIV-1 infection and AIDS who have a known seroconversion date (n = 102).

METHODS

CD4 and CD8 T cell activation marker expression was analysed by FACScan before and after seroconversion (1 and 5 years after seroconversion); T cell proliferation and T cell numbers were also measured. Cox proportional hazard analyses were used to study the predictive value of these parameters for progression to AIDS.

RESULTS

Preseroconversion low CD4 T cell numbers or elevated levels of CD4 T cell activation were associated with increased risk for development of AIDS after HIV-1 seroconversion. Progression to AIDS was associated with loss of both CD4 and CD8 naive T cells. The predictive value of CD8 T cell activation was confirmed and, in addition, in the course of infection low CD4 T cell counts and increasing proportions of dividing CD4 T cells, dividing CD8 T cells or elevated CD4 T cell activation marker expression became independent predictors of progression to AIDS.

CONCLUSIONS

Increased T cell activation has predictive value for HIV-1 disease progression even before seroconversion. These data support the hypothesis that persistent hyperactivation of the immune system may lead to erosion of the naive T cell pool and CD4 T cell depletion.

摘要

背景

HIV-1感染的特征是慢性全身性CD8和CD4 T细胞过度活化,但其生物学效应尚不清楚。

目的

研究HIV-1感染中慢性免疫活化与CD4 T细胞耗竭之间的关系。

设计

对阿姆斯特丹HIV-1感染和艾滋病队列研究中已知血清转化日期的参与者(n = 102)进行前瞻性队列研究。

方法

在血清转化之前和之后(血清转化后1年和5年)通过流式细胞仪分析CD4和CD8 T细胞活化标志物的表达;还测量了T细胞增殖和T细胞数量。使用Cox比例风险分析来研究这些参数对进展为艾滋病的预测价值。

结果

血清转化前低CD4 T细胞数量或CD4 T细胞活化水平升高与HIV-1血清转化后发生艾滋病的风险增加相关。进展为艾滋病与CD4和CD8初始T细胞的丢失有关。CD8 T细胞活化的预测价值得到证实,此外,在感染过程中,低CD4 T细胞计数以及CD4 T细胞、CD8 T细胞分裂比例增加或CD4 T细胞活化标志物表达升高成为进展为艾滋病的独立预测因素。

结论

T细胞活化增加甚至在血清转化之前就对HIV-1疾病进展具有预测价值。这些数据支持免疫系统持续过度活化可能导致初始T细胞库受损和CD4 T细胞耗竭的假说。

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