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人大颗粒淋巴细胞上的CD11a - c/CD18和GP84(LB - 2)黏附分子及其在自然杀伤中的作用

CD11a-c/CD18 and GP84 (LB-2) adhesion molecules on human large granular lymphocytes and their participation in natural killing.

作者信息

Timonen T, Patarroyo M, Gahmberg C G

机构信息

Department of Pathology, University of Helsinki, Finland.

出版信息

J Immunol. 1988 Aug 1;141(3):1041-6.

PMID:2899596
Abstract

Effect of mAb against the CD11a-c, CD18, and GP84 adhesion molecules on the binding and cytotoxicity of human NK cells was studied. The target cells were K562, MOLT-4, Raji, and fresh uncultured autologous endometrial carcinoma cells. Antibodies against adhesion relevant epitopes of CD11a(TA-1/LFA-1), CD11b(Mol/OKM1/Mac1), or CD11c (Leu-M5) did not inhibit NK function. The mAb 60.3 against CD18, the common beta-chain associated to CD11a-c, strongly inhibited both the binding and cytotoxicity of large granular lymphocytes (LGL) against all the target cells tested. Also the antibody LB-2 against the GP84 adhesion molecule inhibited NK function to some degree. 60.3 and LB-2 antibodies exerted an additive effect in the inhibition of both binding and cytotoxicity. However, even this antibody combination did not completely block NK activity, suggesting a heterogeneity of adhesion structures in the NK system. According to both FACS analyses and immunoprecipitation studies, all the tested antibodies recognized either a subpopulation or all of LGL. On the other hand, antibodies against CD11b, CD11c, and LB-2 showed only marginal reactivity with highly purified LGL-free T cells.

摘要

研究了抗CD11a-c、CD18和GP84黏附分子的单克隆抗体对人自然杀伤细胞(NK细胞)结合及细胞毒性的影响。靶细胞为K562、MOLT-4、Raji细胞以及新鲜未培养的自体子宫内膜癌细胞。抗CD11a(TA-1/LFA-1)、CD11b(Mol/OKM1/Mac1)或CD11c(Leu-M5)黏附相关表位的抗体并未抑制NK细胞功能。抗CD18(与CD11a-c相关的共同β链)的单克隆抗体60.3强烈抑制大颗粒淋巴细胞(LGL)对所有受试靶细胞的结合及细胞毒性。同样,抗GP84黏附分子的抗体LB-2也在一定程度上抑制NK细胞功能。60.3和LB-2抗体在抑制结合及细胞毒性方面具有相加作用。然而,即便这种抗体组合也未完全阻断NK细胞活性,这表明NK细胞系统中黏附结构具有异质性。根据荧光激活细胞分选术(FACS)分析及免疫沉淀研究,所有受试抗体均可识别LGL的一个亚群或全部LGL。另一方面,抗CD11b、CD11c及LB-2抗体与高度纯化的无LGL的T细胞仅表现出微弱反应。

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