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原肌球蛋白外显子作为可变剪接的模型。

Tropomyosin exons as models for alternative splicing.

作者信息

Gooding Clare, Smith Christopher W J

机构信息

Department of Biochemistry, University of Cambridge, CB2 1GA, UK.

出版信息

Adv Exp Med Biol. 2008;644:27-42. doi: 10.1007/978-0-387-85766-4_3.

Abstract

Three of the four mammalian tropomyosin (Tm) genes are alternatively spliced, most commonly by mutually exclusive selection from pairs of internal or 3' end exons. Alternative splicing events in the TPM1, 2 and 3 genes have been analysed experimentally in various levels ofdetail. In particular, mutually exclusive exon pairs in the betaTm (TPM2) and alphaTm (TPM1) genes are among the most intensively studied models for striated and smooth muscle specific alternative splicing, respectively. Analysis of these model systems has provided important insights into general mechanisms and strategies of splicing regulation.

摘要

四种哺乳动物原肌球蛋白(Tm)基因中的三种会发生可变剪接,最常见的是通过从内部或3'端外显子对中进行互斥选择。已经在不同详细程度上对TPM1、2和3基因中的可变剪接事件进行了实验分析。特别是,βTm(TPM2)和αTm(TPM1)基因中的互斥外显子对分别是横纹肌和平滑肌特异性可变剪接研究最深入的模型之一。对这些模型系统的分析为剪接调控的一般机制和策略提供了重要见解。

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