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B7-H1在HIV感染中上调,是疾病进展的一种新型替代标志物。

B7-H1 is up-regulated in HIV infection and is a novel surrogate marker of disease progression.

作者信息

Trabattoni Daria, Saresella Marina, Biasin Mara, Boasso Adriano, Piacentini Luca, Ferrante Pasquale, Dong Haidong, Maserati Renato, Shearer Gene M, Chen Lieping, Clerici Mario

机构信息

Chair of Immunolgy, Dipartimento Scienze Precliniche Laboratorio Integrato Tecnologie Avanzate (DISP LITA) Vialba, University of Milano, Milano, Italy.

出版信息

Blood. 2003 Apr 1;101(7):2514-20. doi: 10.1182/blood-2002-10-3065. Epub 2002 Dec 5.

Abstract

The ligation of programmed death-ligand 1 (B7-H1) to T cells results in the preferential production of interleukin 10 (IL-10). We investigated if B7-H1 would be up-regulated in HIV infection, a disease characterized by increased IL-10 production, by measuring B7-H1, B7-1 (CD80), and B7-2 (CD86) expression and mRNA in 36 HIV-infected patients and in 22 healthy controls (HCs). Results showed that (1) B7-H1 expression and mRNA are augmented in cells of HIV patients; (2) increased IL-10 production in these patients is largely induced by B7-H1-expressing CD14(+) cells; (3) an inverse correlation is detected between B7-H1 expression and CD4 counts, whereas the up-regulation of B7-H1 is directly associated with HIV plasma viremia; (4) antiviral therapy results in the parallel down modulation of IL-10 production and B7-H1 expression/synthesis; and (5) B7-H1/CD80 and B7-H1/CD86 mRNA ratios are increased in peripheral blood mononuclear cells (PBMCs) of HIV patients compared with HCs. B7-H1 synthesis and expression are up-regulated in HIV infection, and the degree of dysregulation correlates with the severity of disease. Aberrant antigen presentation by antigen-presenting cells (APCs) that exhibit increased B7-H1 expression and IL-10 production in HIV infection could be responsible for T-lymphocyte unresponsiveness and loss of protective immunity. B7-H1 is a surrogate marker potentially involved in AIDS disease progression.

摘要

程序性死亡配体1(B7-H1)与T细胞结合会导致白细胞介素10(IL-10)优先产生。我们通过检测36例HIV感染患者和22例健康对照者(HCs)的B7-H1、B7-1(CD80)和B7-2(CD86)的表达及mRNA,来研究B7-H1在以IL-10产生增加为特征的HIV感染中是否会上调。结果显示:(1)HIV患者细胞中B7-H1的表达及mRNA增加;(2)这些患者中IL-10产生增加主要由表达B7-H1的CD14(+)细胞诱导;(3)检测到B7-H1表达与CD4细胞计数呈负相关,而B7-H1的上调与HIV血浆病毒血症直接相关;(4)抗病毒治疗导致IL-10产生以及B7-H1表达/合成平行下调;(5)与HCs相比,HIV患者外周血单个核细胞(PBMCs)中B7-H1/CD80和B7-H1/CD86 mRNA比值增加。HIV感染中B7-H1的合成及表达上调,失调程度与疾病严重程度相关。在HIV感染中表现出B7-H1表达增加及IL-10产生的抗原呈递细胞(APC)异常的抗原呈递可能是T淋巴细胞无反应性及保护性免疫丧失的原因。B7-H1是一个可能参与艾滋病疾病进展的替代标志物。

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