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人自然杀伤细胞克隆与靶细胞相互作用中淋巴细胞功能相关抗原-1(LFA-1)抗原的功能特性

Functional characterization of LFA-1 antigens in the interaction of human NK clones and target cells.

作者信息

Schmidt R E, Bartley G, Levine H, Schlossman S F, Ritz J

出版信息

J Immunol. 1985 Aug;135(2):1020-5.

PMID:3924996
Abstract

In the present studies we analyzed the role of LFA-1 antigens in the interaction between NK clones and target cells. The use of various cloned NK cell lines allowed us to analyze homogeneous populations of NK cells which ordinarily comprise only a small fraction of peripheral blood lymphocytes and are extremely heterogeneous with respect to phenotype and specificity. Indirect immunofluorescence with monoclonal antibodies against the alpha (MHM24) and beta (MHM23) chains of the LFA-1 antigen revealed similar patterns of positive reactivity with all NK clones. Both monoclonal antibodies exerted a significant blocking effect on NK cytotoxicity against target cells such as Molt-4 and CEM, whereas the inhibition was very weak against other targets such as K562 and HSB cells. Additive blocking effects were seen when both monoclonal antibodies MHM23 and MHM24 were added to the cytotoxicity assays. When we compared the inhibitory effect of MHM23 and MHM24 on uncultured peripheral blood NK cells and IL 2-activated NK cells, inhibition of cytotoxicity also was found to be primarily dependent on the individual target cells. Thus, the inhibitory activity of anti-LFA-1 antibody was shown to be independent of the phenotypic and functional heterogeneity of the NK clones, activated NK cells, and unstimulated NK cells utilized in these studies. These blocking effects were found to be independent of the LFA-1 antigen expression on the target cell membrane and inhibition occurred only when antibody was bound to the effector cells. Comparison of the effects of anti-LFA-1, anti-T3, and anti-clonotypic antibodies against a Ti-like structure of different NK clones with a mature T cell phenotype demonstrated that each of these antibodies acts on the effector cells in an independent and additive fashion. However, unlike T3 and NKTa antigen, LFA-1 antigen expression is not modulated by cell surface interaction with antibodies specific for this molecule.

摘要

在本研究中,我们分析了淋巴细胞功能相关抗原-1(LFA-1)抗原在自然杀伤(NK)细胞克隆与靶细胞相互作用中的作用。使用各种克隆的NK细胞系使我们能够分析NK细胞的同质群体,这些细胞通常仅占外周血淋巴细胞的一小部分,并且在表型和特异性方面极其异质。用针对LFA-1抗原的α链(MHM24)和β链(MHM23)的单克隆抗体进行间接免疫荧光显示,所有NK细胞克隆的阳性反应模式相似。两种单克隆抗体对NK细胞对诸如莫特-4(Molt-4)和CEM等靶细胞的细胞毒性均具有显著的阻断作用,而对诸如K562和HSB细胞等其他靶细胞的抑制作用则非常弱。当将单克隆抗体MHM23和MHM24都添加到细胞毒性试验中时,观察到了累加阻断效应。当我们比较MHM23和MHM24对未培养的外周血NK细胞和白细胞介素2(IL-2)激活的NK细胞的抑制作用时,发现细胞毒性的抑制也主要取决于各个靶细胞。因此,抗LFA-1抗体的抑制活性显示与本研究中使用的NK细胞克隆、活化的NK细胞和未刺激的NK细胞的表型和功能异质性无关。发现这些阻断效应与靶细胞膜上的LFA-1抗原表达无关,并且仅当抗体与效应细胞结合时才会发生抑制作用。将抗LFA-1、抗T3和抗独特型抗体针对具有成熟T细胞表型的不同NK细胞克隆的类T细胞样结构的作用进行比较,结果表明这些抗体中的每一种都以独立且累加的方式作用于效应细胞。然而,与T3和NKTa抗原不同,LFA-1抗原的表达不会因与该分子特异性抗体的细胞表面相互作用而受到调节。

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