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通过刺激由HML-1单克隆抗体定义的含β7整合素增强CD3诱导的人肠上皮内淋巴细胞激活。

Enhancement of CD3-induced activation of human intestinal intraepithelial lymphocytes by stimulation of the beta 7-containing integrin defined by HML-1 monoclonal antibody.

作者信息

Sarnacki S, Bègue B, Buc H, Le Deist F, Cerf-Bensussan N

机构信息

INSERM U132, Hôpital Necker-Enfants Malades, Paris, France.

出版信息

Eur J Immunol. 1992 Nov;22(11):2887-92. doi: 10.1002/eji.1830221120.

Abstract

Intraepithelial lymphocytes (IEL) form a large population of T cells in close contact with the intestinal lumen and differ from lymphocytes in other lymphoid compartments by their predominant CD8+ phenotype and the strong expression of the recently characterized beta 7-containing integrin defined by the monoclonal antibody (mAb) HML-1. The aim of the present in vitro study was to investigate the possible role of the integrin defined by HML-1 in the activation of human IEL via the CD3-T cell receptor (TcR) pathway. The proliferative response of IEL to optimal concentrations of immobilized OKT3 was found to be similar to that of peripheral blood lymphocytes enriched in CD8+ cells. When co-immobilized with suboptimal concentrations of OKT3, antibodies directed against CD11a, CD29 and the beta 7-containing integrin defined by HML-1 exerted a strong synergistic effect on the proliferative response and on the expression of CD25 and CD71 antigens by human IEL. These data indicate that the CD3-TcR pathway is functional in human IEL and contrast with previous observations suggesting that the CD3-TcR pathway was difficult to elicit in human IEL. Furthermore, the present data show that the immune response of human IEL can be modulated via interactions between integrins expressed by IEL and their respective ligands in the mucosa and suggest that IEL's activation may depend on the level of expression of integrin ligands in the epithelium, particularly of the expression of the as yet unknown ligand for the IEL-specific integrin defined by HML-1.

摘要

上皮内淋巴细胞(IEL)构成了与肠腔紧密接触的大量T细胞群体,它们与其他淋巴区室中的淋巴细胞不同,其主要为CD8 +表型,并且由单克隆抗体(mAb)HML-1定义的最近鉴定的含β7整合素表达强烈。本体外研究的目的是研究由HML-1定义的整合素在通过CD3-T细胞受体(TcR)途径激活人IEL中的可能作用。发现IEL对最佳浓度的固定化OKT3的增殖反应与富含CD8 +细胞的外周血淋巴细胞的增殖反应相似。当与次最佳浓度的OKT3共同固定时,针对CD11a、CD29和由HML-1定义的含β7整合素的抗体对人IEL的增殖反应以及CD25和CD71抗原的表达产生强烈的协同作用。这些数据表明CD3-TcR途径在人IEL中起作用,这与先前的观察结果形成对比,先前的观察结果表明CD3-TcR途径在人IEL中难以引发。此外,目前的数据表明,人IEL的免疫反应可以通过IEL表达的整合素与其在粘膜中的各自配体之间的相互作用来调节,并表明IEL的激活可能取决于上皮中整合素配体的表达水平,特别是由HML-1定义的IEL特异性整合素的未知配体的表达。

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