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人类淋巴细胞再循环的调控。II. 皮肤淋巴细胞相关抗原的差异调控,一种皮肤归巢T细胞的组织选择性归巢受体。

Control of lymphocyte recirculation in man. II. Differential regulation of the cutaneous lymphocyte-associated antigen, a tissue-selective homing receptor for skin-homing T cells.

作者信息

Picker L J, Treer J R, Ferguson-Darnell B, Collins P A, Bergstresser P R, Terstappen L W

机构信息

Department of Pathology, University of Texas Southwestern Medical Center, Dallas 75235-9072.

出版信息

J Immunol. 1993 Feb 1;150(3):1122-36.

PMID:7678617
Abstract

Recent work indicates that a novel homing receptor (HR)/endothelial ligand pair--the cutaneous lymphocyte-associated Ag (CLA) and E-selectin--is involved in targeting a unique skin-associated subpopulation of memory T cells to cutaneous sites of chronic inflammation. To investigate the regulatory mechanisms responsible for the generation of a memory T cell subset with skin-selective homing capability, we used multiparameter flow cytometry to assess the expression of CLA on T cells during initial T cell activation in secondary lymphoid tissues (the virgin to memory transition), and upon reactivation in skin. Our analyses indicate that in vivo induction of CLA (and E-selectin-binding ability) first occurs during the virgin to memory transition, and is regulated in a highly tissue-selective manner. The frequency of CLA expression on CD45RA+/RO+ transitional T cells within skin-associated peripheral lymph nodes was > fivefold higher than within the mucosal microenvironment of the appendix. In keeping with its role as a skin-selective homing receptor, levels of cell-surface CLA on T cells obtained from cutaneous blisters overlying delayed-type hypersensitivity sites were a mean 23-fold higher than on corresponding peripheral blood T cells, including all time points of lesional evolution. However, comparisons of CLA expression on resting vs activated skin blister T cells (HLA-DR - vs +, respectively) indicated that CLA expression, which is already quite high on the resting subset, appeared to be further up-regulated upon activation in skin. The critical involvement of local microenvironments in the regulation of CLA expression was also supported by in vitro studies demonstrating the necessity of specific secondary signals for the induction of CLA glycoproteins on mitogen-activated T cells. CLA up-regulation on both the virgin and memory T cell subsets was dependent on the presence of TGF-beta 1 (or, to a lesser extent, IL-6), but not a wide variety of other cytokines. Thus, the development of the CLA+ memory T cell subset is likely a product of the cumulative experience of those T cells with respect to local microenvironments at previous sites of activation, perhaps involving differential availability of bioactive TGF-beta 1 and/or IL-6 (both cytokines produced in skin). Repeated activation in skin or skin-associated peripheral lymph nodes may act to reinforce CLA expression on T cells functionally-associated with skin, and thus enhance the functional efficiency of these cells by preferentially focusing their recirculation to the skin or related sites.

摘要

近期研究表明,一种新型归巢受体(HR)/内皮配体对——皮肤淋巴细胞相关抗原(CLA)和E选择素——参与将记忆T细胞的独特皮肤相关亚群靶向至慢性炎症的皮肤部位。为了研究负责产生具有皮肤选择性归巢能力的记忆T细胞亚群的调控机制,我们使用多参数流式细胞术来评估在次级淋巴组织中初始T细胞激活期间(从初始T细胞到记忆T细胞的转变)以及在皮肤中再次激活时T细胞上CLA的表达。我们的分析表明,CLA(以及与E选择素结合的能力)在体内的诱导首先发生在从初始T细胞到记忆T细胞的转变过程中,并且以高度组织选择性的方式受到调控。皮肤相关外周淋巴结内CD45RA+/RO+过渡性T细胞上CLA表达的频率比阑尾的黏膜微环境内高五倍以上。与其作为皮肤选择性归巢受体的作用一致,从迟发型超敏反应部位上方的皮肤水疱中获得的T细胞表面CLA水平比相应外周血T细胞平均高23倍,包括病变演变的所有时间点。然而,对静息与激活的皮肤水疱T细胞(分别为HLA-DR - 与 +)上CLA表达的比较表明,静息亚群上已经相当高的CLA表达在皮肤激活后似乎进一步上调。体外研究也支持局部微环境在CLA表达调控中的关键作用,这些研究表明在丝裂原激活的T细胞上诱导CLA糖蛋白需要特定的第二信号。初始T细胞和记忆T细胞亚群上CLA的上调均依赖于TGF-β1(或在较小程度上依赖于IL-6)的存在,但不依赖于多种其他细胞因子。因此,CLA+记忆T细胞亚群的发育可能是这些T细胞在先前激活部位对局部微环境累积体验的产物,可能涉及生物活性TGF-β1和/或IL-6(两者均在皮肤中产生)的不同可用性。在皮肤或皮肤相关外周淋巴结中的反复激活可能会增强与皮肤功能相关的T细胞上CLA的表达,从而通过优先将它们的再循环集中到皮肤或相关部位来提高这些细胞的功能效率。

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