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人记忆/效应T细胞在肺部与皮肤免疫效应部位淋巴细胞归巢受体的差异表达。

Differential expression of lymphocyte homing receptors by human memory/effector T cells in pulmonary versus cutaneous immune effector sites.

作者信息

Picker L J, Martin R J, Trumble A, Newman L S, Collins P A, Bergstresser P R, Leung D Y

机构信息

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

出版信息

Eur J Immunol. 1994 Jun;24(6):1269-77. doi: 10.1002/eji.1830240605.

Abstract

The heterogeneous expression of lymphocyte homing receptors (HR) by the (CD45RA(low)/RO(high)) memory/effector T cell population in the human is thought to define subsets with tissue-selective recirculatory potential. To investigate further the localization characteristics of these T cells, we used multiparameter flow cytometry to quantitate T cell subsets defined by expression of the skin-selective HR called the cutaneous lymphocyte-associated antigen (CLA), the peripheral lymph node (PLN) HR L-selectin, the mucosal-associated HR alpha 4 beta 7-integrin, and the mucosal-associated adhesion molecule alpha e beta 7-integrin in either cutaneous or pulmonary immune effector sites and corresponding peripheral blood. Compared to peripheral blood, skin T cells were highly enriched for the CLA+/L-selectin+/alpha e beta 7-integrin- memory/effector subset, whereas lung memory/effector T cells were predominantly CLA-to low L-selectin-, and almost half were alpha e beta 7-integrin+. alpha 4 beta 7-integrin expressing memory/effector T cells were diminished in both skin and lung, suggesting that this HR is not a major participant in determining localization specificity in either of these sites. The characteristic pulmonary T cell HR phenotype did not significantly differ between the normal subjects and those with pulmonary inflammatory disease, and did not correlate with markers of T cell activation. Induction of a rapid up-regulation of pulmonary inflammation via intrabronchial allergen challenge in asthmatic patients tended to decrease localization specificity, resulting in a more general importation of memory/effector subsets. Taken together, these results suggest that tissue microenvironments play a major role in determining the character of local T cell infiltrates via their ability to import and retain memory/effector subsets selectively or, more generally, depending on the intensity of local inflammatory stimuli.

摘要

人类中(CD45RA(low)/RO(high))记忆/效应T细胞群体淋巴细胞归巢受体(HR)的异质性表达被认为定义了具有组织选择性再循环潜能的亚群。为了进一步研究这些T细胞的定位特征,我们使用多参数流式细胞术来定量由皮肤选择性HR(称为皮肤淋巴细胞相关抗原(CLA))、外周淋巴结(PLN)HR L-选择素、黏膜相关HRα4β7整合素以及黏膜相关黏附分子αeβ7整合素的表达所定义的T细胞亚群,这些亚群存在于皮肤或肺部免疫效应部位以及相应的外周血中。与外周血相比,皮肤T细胞中CLA+/L-选择素+/αeβ7整合素-记忆/效应亚群高度富集,而肺记忆/效应T细胞主要是CLA-至低L-选择素-,并且几乎一半是αeβ7整合素+。表达α4β7整合素的记忆/效应T细胞在皮肤和肺中均减少,这表明该HR不是决定这两个部位中任何一个部位定位特异性的主要参与者。正常受试者和患有肺部炎症疾病的受试者之间,特征性的肺部T细胞HR表型没有显著差异,并且与T细胞活化标志物无关。哮喘患者通过支气管内过敏原激发诱导肺部炎症的快速上调往往会降低定位特异性,导致记忆/效应亚群更普遍的导入。综上所述,这些结果表明组织微环境在决定局部T细胞浸润特征方面起主要作用,其机制是通过有选择地导入和保留记忆/效应亚群的能力,或者更普遍地说,取决于局部炎症刺激的强度。

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