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心脏elav型RNA结合蛋白(ETR-3)与强直性肌营养不良中扩增的RNA CUG重复序列结合。

Cardiac elav-type RNA-binding protein (ETR-3) binds to RNA CUG repeats expanded in myotonic dystrophy.

作者信息

Lu X, Timchenko N A, Timchenko L T

机构信息

Departments of Medicine, Section of Cardiology and Pathology, Baylor College of Medicine, One Baylor Plaza, Houston, TX 77030, USA.

出版信息

Hum Mol Genet. 1999 Jan;8(1):53-60. doi: 10.1093/hmg/8.1.53.

Abstract

Myotonic dystrophy (DM) is a neuromuscular disorder associated with CTG triplet repeat expansion in the myotonin protein kinase gene ( DMPK ). We previously proposed a hypothesis suggesting that the expanded CUG repeats sequester specific RNA-binding proteins and that such a sequestration results in abnormal RNA processing of several RNAs containing CUG repeats in multiple tissues affected in patients with DM. One of the members of the CUG-binding proteins, CUG-BP, has been identified previously. Here we describe the second member of this family, elav -type ribonucleoprotein (ETR-3), which is highly expressed in heart and is able to interact with CUG repeats. Screening of a mouse liver cDNA library with a CUG-BP probe identified two mETR-3 cDNAs. Two additional cDNAs from mouse heart were amplified by RT-PCR. These cDNAs differ by several insertions/deletions and might be generated via alternative splicing. Mouse ETR-3 has a mol. wt of 50 kDa and displays a high level of homology to CUG-BP protein. The organization of the RNA-binding domains (RBDs) within the ETR-3 molecule is similar to one within CUG-BP. A study of mETR-3 RNA-binding activity showed that the mETR-3 binds to (CUG)8repeats. Sequence analysis of mETR-3 indicates the presence of several CUG repeats within the mETR-3 mRNA. Both CUG-BP and mETR-3 bind to mETR-3 mRNA via CUG repeats, suggesting the possible involvement of CUG-BP-like proteins in the regulation of mETR-3 processing. Analysis of the tissue distribution of ETR-3 showed that in human cells, ETR-3 mRNA is highly expressed in heart, but is undetectable in other tissues examined. Our results suggest the existence of a family of proteins that bind to CUG repeats and might be affected in DM by expansion of CUG repeats.

摘要

强直性肌营养不良(DM)是一种神经肌肉疾病,与肌强直性蛋白激酶基因(DMPK)中的CTG三联体重复扩增有关。我们之前提出了一个假说,认为扩增的CUG重复序列会隔离特定的RNA结合蛋白,而这种隔离会导致DM患者多个受影响组织中几种含有CUG重复序列的RNA的异常RNA加工。CUG结合蛋白家族的成员之一CUG-BP,此前已被鉴定。在此,我们描述了该家族的第二个成员,即elav型核糖核蛋白(ETR-3),它在心脏中高度表达,并且能够与CUG重复序列相互作用。用CUG-BP探针筛选小鼠肝脏cDNA文库,鉴定出两个mETR-3 cDNA。通过RT-PCR扩增出另外两个来自小鼠心脏的cDNA。这些cDNA因几个插入/缺失而有所不同,可能是通过可变剪接产生的。小鼠ETR-3的分子量为50 kDa,与CUG-BP蛋白具有高度同源性。ETR-3分子内RNA结合结构域(RBD)的组织方式与CUG-BP内的相似。对mETR-3 RNA结合活性的研究表明,mETR-3与(CUG)8重复序列结合。mETR-3的序列分析表明mETR-3 mRNA内存在几个CUG重复序列。CUG-BP和mETR-3都通过CUG重复序列与mETR-3 mRNA结合,这表明CUG-BP样蛋白可能参与mETR-3加工的调控。对ETR-3组织分布的分析表明,在人类细胞中,ETR-3 mRNA在心脏中高度表达,但在其他检测的组织中未检测到。我们的结果表明存在一个与CUG重复序列结合的蛋白家族,并且可能在DM中因CUG重复序列的扩增而受到影响。

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