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由于缺乏CD3γ导致的T淋巴细胞信号缺陷和免疫缺陷。

T lymphocyte signalling defects and immunodeficiency due to the lack of CD3 gamma.

作者信息

Arnaiz-Villena A, Timon M, Rodriguez-Gallego C, Iglesias-Casarrubios P, Pacheco A, Regueiro J R

机构信息

Department of Immunology, Hospital 12 de Octubre, Madrid, Spain.

出版信息

Immunodeficiency. 1993;4(1-4):121-9.

PMID:7909475
Abstract

A selective CD3 gamma defect, involving point mutations in both the paternal and the maternal genes, has been analyzed. The CD3 gamma defect affected two brothers of a four sibs family; one of them died at the age of 3 of a viral pneumonia with concomitant autoimmune features (Haemolytic anaemia and gut epithelial cell autoantibodies), whereas the other is still alive at the age of 10 with relatively mild infection episodes. In this work, the effects of the absence of the CD3 gamma chain in the structure and signal transduction of the T-cell receptor (TCR)/CD3 complex and in the selection and function of T lymphocytes were studied. The absence of CD3 gamma did not prevent the expression of certain amounts of TCR/CD3 complexes on the surface of T lymphocytes. This suggests the existence of at least two TCR/CD3 isoforms in T cells, either with or without CD3 gamma. A persistent low proportion of CD8+ T cells, not functional in vitro (they were unable to proliferate) and probably in vivo (associated to a lethal viral pneumonia), was observed. In contrast, the proportion of CD4+ T cells was not altered, and they were functional both in vitro (they showed a normal proliferation and a low, but detectable, increase of cytosolic Ca2+ in response to anti-TCR/CD3 stimuli, although the production of IL-2 was impaired) and in vitro (they normally helped B cells). These results show that the absence of CD3 gamma affects the selection and function of cytotoxic, but apparently not helper, T lymphocytes, although the possibility that the CD4+ T cells represent a specific subpopulation can not be ruled out. They also suggest that the interactions of the TCR/CD3 complex with its co-receptors during thymic selection and antigen recognition in the periphery may be asymmetrical, with CD8 interacting through CD3 gamma and, probably, CD4 through the homologous CD3 delta.

摘要

已对一种选择性CD3γ缺陷进行了分析,该缺陷涉及父本和母本基因中的点突变。CD3γ缺陷影响了一个四口之家的两个兄弟;其中一人在3岁时死于伴有自身免疫特征(溶血性贫血和肠道上皮细胞自身抗体)的病毒性肺炎,而另一人在10岁时仍然存活,感染发作相对较轻。在这项研究中,研究了CD3γ链缺失对T细胞受体(TCR)/CD3复合物的结构和信号转导以及T淋巴细胞的选择和功能的影响。CD3γ的缺失并未阻止T淋巴细胞表面表达一定量的TCR/CD3复合物。这表明T细胞中至少存在两种TCR/CD3异构体,一种有CD3γ,另一种没有。观察到CD8 + T细胞比例持续较低,在体外无功能(它们无法增殖),在体内可能也无功能(与致命的病毒性肺炎相关)。相比之下,CD4 + T细胞的比例没有改变,它们在体外(它们表现出正常增殖,并且在抗TCR/CD3刺激下胞质Ca2 +有低但可检测到的增加,尽管IL-2的产生受损)和体内(它们正常辅助B细胞)均有功能。这些结果表明,CD3γ的缺失影响细胞毒性T淋巴细胞的选择和功能,但显然不影响辅助性T淋巴细胞,尽管不能排除CD4 + T细胞代表特定亚群的可能性。它们还表明,在胸腺选择和外周抗原识别过程中,TCR/CD3复合物与其共受体的相互作用可能是不对称的,CD8通过CD3γ相互作用,可能CD4通过同源的CD3δ相互作用。

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