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对突变体表型和剪接缺陷的分析表明,在体内,必需剪接因子U2AF的大亚基和小亚基之间存在功能协作。

Analysis of mutant phenotypes and splicing defects demonstrates functional collaboration between the large and small subunits of the essential splicing factor U2AF in vivo.

作者信息

Webb Christopher J, Lakhe-Reddy Sujata, Romfo Charles M, Wise Jo Ann

机构信息

Department of Molecular Biology and Microbiology, School of Medicine, Case Western Reserve University, Cleveland, OH 44106-4960, USA.

出版信息

Mol Biol Cell. 2005 Feb;16(2):584-96. doi: 10.1091/mbc.e04-09-0768. Epub 2004 Nov 17.

Abstract

The heterodimeric splicing factor U2AF plays an important role in 3' splice site selection, but the division of labor between the two subunits in vivo remains unclear. In vitro assays led to the proposal that the human large subunit recognizes 3' splice sites with extensive polypyrimidine tracts independently of the small subunit. We report in vivo analysis demonstrating that all five domains of spU2AFLG are essential for viability; a partial deletion of the linker region, which forms the small subunit interface, produces a severe growth defect and an aberrant morphology. A small subunit zinc-binding domain mutant confers a similar phenotype, suggesting that the heterodimer functions as a unit during splicing in Schizosaccharomyces pombe. As this is not predicted by the model for metazoan 3' splice site recognition, we sought introns for which the spU2AFLG and spU2AFSM make distinct contributions by analyzing diverse splicing events in strains harboring mutations in each partner. Requirements for the two subunits are generally parallel and, moreover, do not correlate with the length or strength of the 3' pyrimidine tract. These and other studies performed in fission yeast support a model for 3' splice site recognition in which the two subunits of U2AF functionally collaborate in vivo.

摘要

异二聚体剪接因子U2AF在3'剪接位点选择中起重要作用,但两个亚基在体内的分工仍不清楚。体外实验表明,人类大亚基可独立于小亚基识别具有广泛多嘧啶序列的3'剪接位点。我们的体内分析报告显示,裂殖酵母U2AF大亚基(spU2AFLG)的所有五个结构域对细胞存活至关重要;形成小亚基界面的连接区部分缺失会导致严重的生长缺陷和异常形态。小亚基锌结合结构域突变体表现出类似的表型,这表明在裂殖酵母剪接过程中,异二聚体作为一个整体发挥作用。由于后生动物3'剪接位点识别模型无法预测这一现象,我们通过分析每个亚基发生突变的菌株中的不同剪接事件,寻找spU2AFLG和裂殖酵母U2AF小亚基(spU2AFSM)发挥不同作用的内含子。两个亚基的需求通常是平行的,而且与3'嘧啶序列的长度或强度无关。在裂殖酵母中进行的这些研究及其他研究支持了一种3'剪接位点识别模型,即U2AF的两个亚基在体内进行功能协作。

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