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T细胞受体(α、β、γ)基因重排在正常及白血病大颗粒淋巴细胞/自然杀伤细胞中的重排及表达

T cell receptor (alpha, beta, gamma) gene rearrangements and expression in normal and leukemic large granular lymphocytes/natural killer cells.

作者信息

Pelicci P G, Allavena P, Subar M, Rambaldi A, Pirelli A, Di Bello M, Barbui T, Knowles D M, Dalla-Favera R, Mantovani A

机构信息

Department of Pathology, New York University School of Medicine, New York.

出版信息

Blood. 1987 Nov;70(5):1500-8.

PMID:2444290
Abstract

The large granular lymphocyte (LGL) population, which effects a natural killer (NK) function, consists of cells whose lineage derivation has not been clearly established on the basis of phenotypic and functional properties. To clarify the relationship of LGL/NK cells to T cells we studied patterns of rearrangement and expression of the T cell receptor (Ti) genes alpha, beta, and gamma in normal human LGLs; in CD8+, CD8-, Mol+, and Mol- LGL subsets; and in 17 cases of leukemic LGL proliferations (T gamma LPD). T alpha, T beta, and T gamma genes were not expressed, nor were T beta and T gamma genes rearranged in normal LGLs or LGL subsets. The T gamma LPD were divided into two groups. One group (15/17 cases) was characterized as CD3+ and displayed Ti gene rearrangements. Seven of these cases were reactive with monoclonal antibody WT31, which suggested expression of an alpha/beta heterodimer on the cell surface. The other group (2/17 cases) was CD3- with unrearranged Ti genes. These results indicate that the normal LGL/NK population is homogeneous and distinct from the normal T cell population because it does not express, and as a result, cannot effect its immune function through the T cell receptor molecules. Conversely, T gamma LPDs represent a heterogeneous group of lymphoproliferative diseases within which the CD3-, Ti- cases most likely represent the neoplastic counterpart of normal LGL cells. The more frequent CD3+ cases may be related to recently described NK-like T cells. The observations that normal LGLs maintain germline T gamma genes and that many CD3+ T gamma LPD display an alpha/beta heterodimer suggest that a T gamma-containing receptor may not be necessary for NK or NK-like cytotoxicity.

摘要

具有自然杀伤(NK)功能的大颗粒淋巴细胞(LGL)群体,由那些根据表型和功能特性其谱系来源尚未明确确定的细胞组成。为了阐明LGL/NK细胞与T细胞的关系,我们研究了正常人LGL中、CD8 +、CD8 -、Mol +和Mol - LGL亚群中以及17例白血病性LGL增殖(TγLPD)中T细胞受体(Ti)基因α、β和γ的重排和表达模式。正常LGL或LGL亚群中未表达Tα、Tβ和Tγ基因,Tβ和Tγ基因也未重排。TγLPD分为两组。一组(15/17例)的特征为CD3 +并显示Ti基因重排。其中7例与单克隆抗体WT31反应,提示细胞表面表达α/β异二聚体。另一组(2/17例)为CD3 -且Ti基因未重排。这些结果表明,正常LGL/NK群体是同质的,且与正常T细胞群体不同,因为它不表达,因此不能通过T细胞受体分子发挥其免疫功能。相反,TγLPD代表一组异质性的淋巴增殖性疾病,其中CD3 -、Ti -的病例很可能代表正常LGL细胞的肿瘤对应物。更常见的CD3 +病例可能与最近描述的NK样T细胞有关。正常LGL维持Tγ基因种系以及许多CD3 + TγLPD显示α/β异二聚体的观察结果表明,含Tγ的受体可能不是NK或NK样细胞毒性所必需的。

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