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肠道上皮内淋巴细胞亚群的差异功能。

Differential function of intestinal intraepithelial lymphocyte subsets.

作者信息

Barrett T A, Gajewski T F, Danielpour D, Chang E B, Beagley K W, Bluestone J A

机构信息

Ben May Institute, University of Chicago, IL 60637.

出版信息

J Immunol. 1992 Aug 15;149(4):1124-30.

PMID:1380032
Abstract

It has been proposed that intestinal intraepithelial lymphocytes (I-IEL) perform immune surveillance of the epithelial layer (1) and regulate mucosal humoral responses to exogenous Ag (2). To better understand the functional potential of this unique population, purified murine I-IEL were analyzed phenotypically and functionally. Initial studies determined that I-IEL could be distinguished based on several phenotypic characteristics including: TCR (TCR-alpha beta vs TCR-gamma delta); Thy-1, CD45R/B220, CD5, and CD8 (CD8 alpha alpha vs CD8 alpha beta) expression. Using anti-TCR mAb, individual I-IEL subsets were activated and examined functionally. Both TCR-alpha beta and TCR-gamma delta I-IEL were found to synthesize an array of lymphokines that included IL-2, IL-3, and IL-6 but not IL-4 or IL-5. Additionally, a number of lymphokines were detected that directly influence epithelial function (IFN-gamma, TNF-alpha, and TGF-beta 1). However, the majority of the I-IEL function was localized within the Thy-1+, CD45R/B220- I-IEL subset. In addition those TCR-alpha beta I-IEL expressing the CD8 alpha beta heterodimer were more easily activated. Thus, a subset of I-IEL have the capacity to respond to TCR-mediated stimuli. The functional activities of these cells may influence both local immune cell populations as well as epithelial differentiation.

摘要

有人提出,肠道上皮内淋巴细胞(I-IEL)对上皮层进行免疫监视(1),并调节黏膜对外源抗原的体液反应(2)。为了更好地了解这一独特细胞群体的功能潜力,对纯化的小鼠I-IEL进行了表型和功能分析。初步研究确定,I-IEL可根据多种表型特征进行区分,包括:TCR(TCR-αβ与TCR-γδ);Thy-1、CD45R/B220、CD5和CD8(CD8αα与CD8αβ)的表达。使用抗TCR单克隆抗体,激活单个I-IEL亚群并进行功能检测。发现TCR-αβ和TCR-γδ I-IEL均能合成一系列细胞因子,包括IL-2、IL-3和IL-6,但不包括IL-4或IL-5。此外,还检测到一些直接影响上皮功能的细胞因子(IFN-γ、TNF-α和TGF-β1)。然而,大多数I-IEL功能定位于Thy-1+、CD45R/B220-I-IEL亚群内。此外,那些表达CD8αβ异二聚体的TCR-αβ I-IEL更容易被激活。因此,一部分I-IEL有能力对TCR介导的刺激作出反应。这些细胞的功能活动可能会影响局部免疫细胞群体以及上皮分化。

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