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可变剪接限制了T细胞受体δ/α基因座重排的翻译。

Alternative splicing restricts translation of rearrangements at the T-cell receptor delta/alpha locus.

作者信息

Hansen-Hagge T E, Mahotka C, Panzer-Grümayer R E, Reuter H J, Schwarz K, van Dongen J J, Bartram C R

机构信息

Department of Pediatrics II, University of Ulm, Germany.

出版信息

Blood. 1995 Apr 1;85(7):1888-96.

PMID:7535593
Abstract

Lymphocytes expressing alpha beta or gamma delta T-cell receptors (TCR) represent distinct T-cell populations. Because TCR delta genes lie within the TCR alpha locus, the rearrangement processes, transcription, and translation of TCR delta or TCR alpha variable domain exons require tight regulation. Human precursor B-cell leukemias (eg, the REH cell line) constitute an interesting model to study TCR delta/alpha recombination because they rearrange TCR delta/alpha loci along a hierarchically ordered pathway in which V delta 2D delta 3 segments are joined to the J alpha cluster. We now show for REH cells that chimeric TCR delta/alpha variable domain exons are posttranscriptionally modified by alternative splicing resulting in truncated V delta 2C alpha transcripts. This process also takes place during thymic differentiation. CD7+/CD3- T-cell precursors exhibit V delta 2D delta 3 rearrangements. Further differentiation into CD7+/CD3+ thymocytes is associated with the expression of a truncated V delta 2C alpha RNA species. In contrast, chimeric TCR delta/alpha rearrangements containing a V delta 1 segment (but no D delta sequences) are predominantly expressed as full-length V delta 1J alpha C alpha transcripts. These data suggest that alternative splicing constitutes a mechanism that restricts the production of distinct chimeric TCR alpha chains.

摘要

表达αβ或γδ T细胞受体(TCR)的淋巴细胞代表不同的T细胞群体。由于TCRδ基因位于TCRα基因座内,TCRδ或TCRα可变结构域外显子的重排过程、转录和翻译需要严格调控。人类前体B细胞白血病(如REH细胞系)构成了一个研究TCRδ/α重组的有趣模型,因为它们沿着层次有序的途径重排TCRδ/α基因座,其中Vδ2Dδ3片段与Jα簇相连。我们现在发现,对于REH细胞,嵌合的TCRδ/α可变结构域外显子通过可变剪接进行转录后修饰,产生截短的Vδ2Cα转录本。这个过程也发生在胸腺分化过程中。CD7+/CD3- T细胞前体表现出Vδ2Dδ3重排。进一步分化为CD7+/CD3+胸腺细胞与截短的Vδ2Cα RNA种类的表达相关。相反,包含Vδ1片段(但无Dδ序列)的嵌合TCRδ/α重排主要表达为全长Vδ1JαCα转录本。这些数据表明可变剪接构成了一种限制不同嵌合TCRα链产生的机制。

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