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FoxP3high 调节性 T 细胞的高周转率与慢性 HIV-1 感染的过度激活和疾病进展相关。

Increased turnover of FoxP3high regulatory T cells is associated with hyperactivation and disease progression of chronic HIV-1 infection.

机构信息

Center for Infection and Immunity, Institute of Biophysics, Chinese Academy of Sciences, Beijing, China.

出版信息

J Acquir Immune Defic Syndr. 2010 Aug;54(5):455-62. doi: 10.1097/QAI.0b013e3181e453b9.

DOI:10.1097/QAI.0b013e3181e453b9
PMID:20585263
Abstract

OBJECTIVES

To characterize the homeostasis of CD4FoxP3 regulatory T cells (Treg) and its association with immune hyperactivation in the disease progression of chronic HIV-1 infection.

DESIGN

Treg proliferation and apoptosis markers were determined and the relation to disease progression and Treg activation was analyzed.

METHODS

Fifty-six HIV-1-infected highly active antiretroviral therapy (HAART)-naive subjects and 17 HAART-treated subjects were enrolled. Proliferation and apoptosis of Treg from peripheral blood were evaluated by intracellular Ki-67 and active caspase-3 or surface Annexin-V staining. T-cell activation markers, CD38 and HLA-DR, were simultaneously monitored. The effects of in vitro TCR (T cell receptor) stimulation on proliferation, apoptosis, and activation of Treg were determined from both HIV-1-infected subjects and healthy controls.

RESULTS

HIV-1-infected patients displayed increased Treg turnover status indicated by higher expression of proliferation marker Ki-67 and apoptosis marker active caspase-3 and Annexin-V. Turnover level of Treg was positively associated with disease progression and immune hyperactivation. In vitro TCR stimulation increased the turnover level of Treg. The HAART treatment decreased the turnover and activation levels of Treg in complete responders.

CONCLUSIONS

Turnover level of Treg was increased in HIV-1-infected subjects, which is associated with immune hyperactivation and the disease progression, and may serve as a surrogate marker to predict HIV-1 disease progression.

摘要

目的

描述 CD4FoxP3 调节性 T 细胞(Treg)的体内平衡及其与慢性 HIV-1 感染疾病进展中免疫过度激活的关系。

设计

测定 Treg 增殖和凋亡标志物,并分析其与疾病进展和 Treg 激活的关系。

方法

纳入 56 例 HIV-1 感染的、未经高效抗逆转录病毒治疗(HAART)的初治患者和 17 例接受 HAART 治疗的患者。通过细胞内 Ki-67 和活性 caspase-3 或表面 Annexin-V 染色评估外周血 Treg 的增殖和凋亡。同时监测 T 细胞活化标志物 CD38 和 HLA-DR。从 HIV-1 感染患者和健康对照者中确定体外 TCR(T 细胞受体)刺激对 Treg 增殖、凋亡和激活的影响。

结果

HIV-1 感染患者的 Treg 周转率升高,表现为增殖标志物 Ki-67 和凋亡标志物活性 caspase-3 和 Annexin-V 的表达增加。Treg 的周转率水平与疾病进展和免疫过度激活呈正相关。体外 TCR 刺激增加了 Treg 的周转率。HAART 治疗降低了完全应答者 Treg 的周转率和激活水平。

结论

HIV-1 感染患者的 Treg 周转率升高,与免疫过度激活和疾病进展相关,可作为预测 HIV-1 疾病进展的替代标志物。

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