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小鼠脑微血管内皮细胞和平滑肌/周细胞对Th1和Th2 CD4 +细胞的差异性激活

Differential activation of Th1 and Th2 CD4+ cells by murine brain microvessel endothelial cells and smooth muscle/pericytes.

作者信息

Fabry Z, Sandor M, Gajewski T F, Herlein J A, Waldschmidt M M, Lynch R G, Hart M N

机构信息

Department of Pathology, University of Iowa College of Medicine, Iowa City 52242.

出版信息

J Immunol. 1993 Jul 1;151(1):38-47.

PMID:8100844
Abstract

CD4+ Th cell infiltration into the brain and the activation by cellular elements of the central nervous system (CNS) are thought to be important steps in the initiation of CNS autoimmune diseases. T cell activation requires Ag-specific stimulation and additional costimulatory signals provided by the APC. Here we describe how murine brain microvessel endothelial (En) cells and smooth muscle/pericytes (SM/P) selectively induce the Ag-specific activation of different Th1 and Th2 CD4+ T cell clones. Th1 and Th2 cell clones were used that were specific for the same peptide Ag in the context of the same class II allotype. SM/P preferentially activated Th1 cell clones, whereas En cells activated Th2 cell clones better, as reflected by cell proliferation and production of IL-2 by SM/P-activated Th1 clones and IL-4 by Th2 clones. There was no difference in the level of expression of CD4, CD2, or LFA-1 molecules between these Th cell clones, and anti-CD4, CD2, LFA-1 or ICAM-1 mAb did not differentially affect Ag-induced proliferation among the clones. Moreover, antibody to CD28 did not influence Ag presentation by brain microvessel En or SM/P cells to Ag-specific Th1 and Th2 clones. These results suggest that: 1) different The subsets might require different signals for their activation; 2) different APC might provide different costimulatory signals for Th cell subsets; and 3) brain microvessel En and SM/P might play a differential role in induction of autoreactive T cell responses in the CNS.

摘要

CD4+辅助性T细胞浸润入脑以及被中枢神经系统(CNS)的细胞成分激活被认为是CNS自身免疫性疾病起始过程中的重要步骤。T细胞激活需要抗原特异性刺激以及抗原呈递细胞(APC)提供的额外共刺激信号。在此我们描述了小鼠脑微血管内皮(En)细胞和平滑肌/周细胞(SM/P)如何选择性地诱导不同的Th1和Th2 CD4+ T细胞克隆的抗原特异性激活。使用了在相同的II类同种异型背景下对相同肽抗原特异的Th1和Th2细胞克隆。SM/P优先激活Th1细胞克隆,而En细胞能更好地激活Th2细胞克隆,这通过SM/P激活的Th1克隆的细胞增殖和IL-2产生以及Th2克隆的IL-4产生得以体现。这些Th细胞克隆之间CD4、CD2或LFA-1分子的表达水平没有差异,抗CD4、CD2、LFA-1或ICAM-1单克隆抗体对克隆间抗原诱导的增殖没有差异影响。此外,抗CD28抗体不影响脑微血管En或SM/P细胞向抗原特异性Th1和Th2克隆的抗原呈递。这些结果表明:1)不同的Th亚群可能需要不同的信号来激活;2)不同的APC可能为Th细胞亚群提供不同的共刺激信号;3)脑微血管En和SM/P可能在CNS自身反应性T细胞应答的诱导中发挥不同作用。

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