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通过可变剪接对异质性核糖核蛋白L蛋白进行自身调节和交叉调节。

Auto- and cross-regulation of the hnRNP L proteins by alternative splicing.

作者信息

Rossbach Oliver, Hung Lee-Hsueh, Schreiner Silke, Grishina Inna, Heiner Monika, Hui Jingyi, Bindereif Albrecht

机构信息

Institute of Biochemistry, Justus-Liebig-University of Giessen, Giessen, Germany.

出版信息

Mol Cell Biol. 2009 Mar;29(6):1442-51. doi: 10.1128/MCB.01689-08. Epub 2009 Jan 5.

DOI:10.1128/MCB.01689-08
PMID:19124611
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2648227/
Abstract

We recently characterized human hnRNP L as a global regulator of alternative splicing, binding to CA-repeat and CA-rich elements. Here we report that hnRNP L autoregulates its own expression on the level of alternative splicing. Intron 6 of the human hnRNP L gene contains a short exon that, if used, introduces a premature termination codon, resulting in nonsense-mediated decay (NMD). This "poison exon" is preceded by a highly conserved CA-rich cluster extending over 800 nucleotides that binds hnRNP L and functions as an unusually extended, intronic enhancer, promoting inclusion of the poison exon. As a result, excess hnRNP L activates NMD of its own mRNA, thereby creating a negative autoregulatory feedback loop and contributing to homeostasis of hnRNP L levels. We present experimental evidence for this mechanism, based on NMD inactivation, hnRNP L binding assays, and hnRNP L-dependent alternative splicing of heterologous constructs. In addition, we demonstrate that hnRNP L cross-regulates inclusion of an analogous poison exon in the hnRNP L-like pre-mRNA, which explains the reciprocal expression of the two closely related hnRNP L proteins.

摘要

我们最近将人类hnRNP L鉴定为可变剪接的全局调节因子,它与CA重复序列和富含CA的元件结合。在此我们报告,hnRNP L在可变剪接水平上对自身表达进行自动调节。人类hnRNP L基因的内含子6包含一个短外显子,如果使用该外显子,会引入一个提前终止密码子,导致无义介导的衰变(NMD)。这个“毒性外显子”之前有一个高度保守的富含CA的簇,延伸超过800个核苷酸,该簇结合hnRNP L并作为一个异常延伸的内含子增强子发挥作用,促进毒性外显子的包含。结果,过量的hnRNP L激活其自身mRNA的NMD,从而形成一个负向自动调节反馈环,并有助于hnRNP L水平的稳态。我们基于NMD失活、hnRNP L结合测定以及异源构建体的hnRNP L依赖性可变剪接,为这一机制提供了实验证据。此外,我们证明hnRNP L交叉调节hnRNP L样前体mRNA中类似毒性外显子的包含,这解释了两种密切相关的hnRNP L蛋白的相互表达。

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