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CD3 阴性和 CD3 阳性 CD56 阳性细胞的比较研究:形态学、功能、T 细胞受体重排及成孔蛋白表达检测

Comparative studies of CD3- and CD3+ CD56+ cells: examination of morphology, functions, T cell receptor rearrangement, and pore-forming protein expression.

作者信息

Ortaldo J R, Winkler-Pickett R T, Yagita H, Young H A

机构信息

Laboratory of Experimental Immunology, National Cancer Institute, Frederick, Maryland 21702-1201.

出版信息

Cell Immunol. 1991 Sep;136(2):486-95. doi: 10.1016/0008-8749(91)90369-m.

DOI:10.1016/0008-8749(91)90369-m
PMID:1714795
Abstract

Both CD3- and CD3+ CD56+ effector cells can mediate non-MHC-restricted lysis in the absence of activation. Previous studies have shown that both of these subsets can be augmented with IL-2. In the present study, we have examined further the phenotypic markers expressed on these cells as well as the functional capacities of these subsets, including LAK activity, cytokine expression, and pore-forming protein (PFP) production. In addition, these populations were analyzed for clonality by Southern blot analysis of the T cell receptor beta chain gene constant region. The CD3-, CD56+ and CD3+, CD56+ lymphocytes were quite similar in their phenotypic markers, although the CD3+, CD56+ lymphocytes lacked high levels of IL-2 receptor beta chain and did not express CD16. The CD3+, CD56+ lymphocytes mediated non-MHC-restricted lysis, but failed to express LAK activity or be induced by IL-2 to secrete IFN gamma, a characteristic of the CD3-, CD56+ lymphocytes. The T cell receptor beta chain gene pattern of the CD3+, CD56+ lymphocytes was characteristic of a polyclonal cell population. Of interest, both populations of cells appeared morphologically to be large granular lymphocytes that contain PFP in their cytoplasmic granules. Therefore these CD56+ subsets provide a new model to study several questions related to non-MHC-restricted target cell lysis, including the identification of novel receptors involved in target cell recognition and/or triggering as well as the biochemical pathways implicated in cellular lysis.

摘要

CD3 - 和CD3 + CD56 +效应细胞在未激活的情况下均可介导非MHC限制的细胞溶解。先前的研究表明,这两个亚群均可被IL - 2增强。在本研究中,我们进一步研究了这些细胞上表达的表型标志物以及这些亚群的功能能力,包括LAK活性、细胞因子表达和孔形成蛋白(PFP)的产生。此外,通过对T细胞受体β链基因恒定区的Southern印迹分析来分析这些群体的克隆性。CD3 - 、CD56 +和CD3 + 、CD56 +淋巴细胞在表型标志物方面非常相似,尽管CD3 + 、CD56 +淋巴细胞缺乏高水平的IL - 2受体β链且不表达CD16。CD3 + 、CD56 +淋巴细胞介导非MHC限制的细胞溶解,但未能表达LAK活性,也不能被IL - 2诱导分泌IFNγ,而这是CD3 - 、CD56 +淋巴细胞的一个特征。CD3 + 、CD56 +淋巴细胞的T细胞受体β链基因模式具有多克隆细胞群体的特征。有趣的是,这两种细胞群体在形态上似乎都是大颗粒淋巴细胞,其细胞质颗粒中含有PFP。因此,这些CD56 +亚群为研究与非MHC限制的靶细胞溶解相关的几个问题提供了一个新模型,包括鉴定参与靶细胞识别和/或触发的新型受体以及与细胞溶解有关的生化途径。

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