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TCR基因重组与αβ-γδ谱系分化:有功能的TCR-β重排既不是γδ细胞发育的唯一条件,也不是其发育的排除条件。

TCR gene recombination and alpha beta-gamma delta lineage divergence: productive TCR-beta rearrangement is neither exclusive nor preclusive of gamma delta cell development.

作者信息

Burtrum D B, Kim S, Dudley E C, Hayday A C, Petrie H T

机构信息

Immunology Program, Memorial Sloan-Kettering Cancer Center, New York 10021, USA.

出版信息

J Immunol. 1996 Nov 15;157(10):4293-6.

PMID:8906802
Abstract

Two types of T lymphocytes can be generated intrathymically, distinguishable by either TCR-gamma delta or -alpha beta surface expression. Regulation of the intrathymic divergence of these cells is unresolved, at least in part because thymically derived gamma delta cells have rarely been studied. We used quantitative Southern blotting together with PCR-based cloning/sequencing and restriction fragment length polymorphism to analyze TCR-alpha and -beta gene recombination in thymically derived gamma delta cells. We found that TCR-beta gene recombination is a frequent occurrence in thymic gamma delta cells. Furthermore, not only do complete (V-D-J) TCR-beta gene rearrangements occur in thymic gamma delta cells, but the frequency of in-frame rearrangements is greater than would be predicted based upon random occurrence. In contrast, we show that thymically derived gamma delta cells do not make detectable rearrangements of the TCR-alpha locus. These studies clearly demarcate a point for alpha beta vs gamma delta commitment in the thymus, after TCR-beta but before TCR-alpha gene recombination. Further, while our data support gamma delta lineage commitment as a consequence of successful TCR-gamma and -delta gene rearrangement, we do not find support for a competitive model of lineage commitment, since productive TCR-beta gene rearrangement does not necessarily relegate cells to the alpha beta lineage.

摘要

胸腺内可产生两种类型的T淋巴细胞,可通过TCR-γδ或-αβ表面表达加以区分。这些细胞在胸腺内分化的调控机制尚未明确,至少部分原因是胸腺来源的γδ细胞很少被研究。我们运用定量Southern印迹法,结合基于PCR的克隆/测序以及限制性片段长度多态性分析,来研究胸腺来源的γδ细胞中TCR-α和-β基因的重组情况。我们发现,TCR-β基因重组在胸腺γδ细胞中频繁发生。此外,胸腺γδ细胞不仅会发生完整的(V-D-J)TCR-β基因重排,而且符合读框的重排频率高于基于随机发生情况所预测的频率。相比之下,我们发现胸腺来源的γδ细胞不会发生可检测到的TCR-α基因座重排。这些研究明确界定了胸腺中αβ与γδ细胞分化的一个关键点,即发生在TCR-β基因重组之后、TCR-α基因重组之前。此外,虽然我们的数据支持γδ细胞系分化是成功进行TCR-γ和-δ基因重排的结果,但我们并未找到支持细胞系分化竞争模型的证据,因为有效的TCR-β基因重排并不一定会使细胞归属于αβ细胞系。

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