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T细胞受体α基因的复杂调控:三种不同的触发诱导模式。

Complex regulation of the T cell receptor alpha gene: three different modes of triggering induction.

作者信息

Wilkinson M F, MacLeod C L

机构信息

Department of Medicine, UCSD Cancer Center, La Jolla, CA 92093-0812.

出版信息

Eur J Immunol. 1988 Jun;18(6):873-9. doi: 10.1002/eji.1830180607.

Abstract

The T cell receptor (TcR) for antigen is composed of variable alpha and beta subunits in noncovalent association with the invariant T3 multimer. TcR/T3 transcripts accumulate in a specific sequence during T cell development; TcR alpha transcripts are the last in the series to accumulate. To explore the regulation of TcR alpha gene expression, we investigated a T lymphoma cell clone which constitutively expresses TcR beta, T3 delta and T3 epsilon mRNA, but essentially lacks detectable TcR alpha mRNA. The cell clone can be induced to accumulate substantial amounts of TcR alpha mRNA in response to phorbol myristate acetate (PMA) or calcium ionophore A23187. Two different protein synthesis inhibitors also induce TcR alpha mRNA. The following evidence indicates that PMA, A23187 and cycloheximide induce TcR alpha by different mechanisms: (a) treatment with a combination of two agents induces greater than additive amounts of TcR alpha mRNA than that induced by a single agent; (b) the immunosuppressant cyclosporin A specifically inhibits A23187-mediated TcR alpha mRNA induction, whereas it fails to inhibit PMA or cycloheximide-mediated induction; and (c) both A23187 and PMA increase the rate of TcR alpha gene transcription, while cycloheximide influences TcR alpha mRNA accumulation by post-transcriptional mechanisms.

摘要

抗原的T细胞受体(TcR)由可变的α和β亚基组成,它们与恒定的T3多聚体以非共价方式结合。在T细胞发育过程中,TcR/T3转录本按特定顺序积累;TcRα转录本是该系列中最后积累的。为了探究TcRα基因表达的调控机制,我们研究了一个T淋巴瘤细胞克隆,该克隆组成性表达TcRβ、T3δ和T3ε mRNA,但基本上检测不到TcRα mRNA。该细胞克隆可被佛波酯肉豆蔻酸酯乙酸盐(PMA)或钙离子载体A23187诱导积累大量的TcRα mRNA。两种不同的蛋白质合成抑制剂也能诱导TcRα mRNA。以下证据表明,PMA、A23187和环己酰亚胺通过不同机制诱导TcRα:(a)用两种试剂联合处理诱导的TcRα mRNA量比单一试剂诱导的量更大;(b)免疫抑制剂环孢素A特异性抑制A23187介导的TcRα mRNA诱导,而它不能抑制PMA或环己酰亚胺介导的诱导;(c)A23187和PMA都增加了TcRα基因的转录速率,而环己酰亚胺通过转录后机制影响TcRα mRNA的积累。

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