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剪接因子hSlu7含有一个将该蛋白质保留在细胞核内所需的独特功能域。

Splicing factor hSlu7 contains a unique functional domain required to retain the protein within the nucleus.

作者信息

Shomron Noam, Reznik Mika, Ast Gil

机构信息

Department of Human Genetics and Molecular Medicine, Sackler School of Medicine, Tel Aviv University, Tel Aviv, Israel 69978.

出版信息

Mol Biol Cell. 2004 Aug;15(8):3782-95. doi: 10.1091/mbc.e04-02-0152. Epub 2004 Jun 4.

Abstract

Precursor-mRNA splicing removes the introns and ligates the exons to form a mature mRNA. This process is carried out in a spliceosomal complex containing >150 proteins and five small nuclear ribonucleoproteins. Splicing protein hSlu7 is required for correct selection of the 3' splice site. Here, we identify by bioinformatics and mutational analyses three functional domains of the hSlu7 protein that have distinct roles in its subcellular localization: a nuclear localization signal, a zinc-knuckle motif, and a lysine-rich region. The zinc-knuckle motif is embedded within the nuclear localization signal in a unique functional structure that is not required for hSlu7's entrance into the nucleus but rather to maintain hSlu7 inside it, preventing its shuttle back to the cytoplasm via the chromosomal region maintenance 1 pathway. Thus, the zinc-knuckle motif of hSlu7 determines the cellular localization of the protein through a nucleocytoplasmic-sensitive shuttling balance. Altogether, this indicates that zinc-dependent nucleocytoplasmic shuttling might be the possible molecular basis by which hSlu7 protein levels are regulated within the nucleus.

摘要

前体mRNA剪接去除内含子并连接外显子以形成成熟的mRNA。这一过程在一个包含超过150种蛋白质和五种小核核糖核蛋白的剪接体复合物中进行。剪接蛋白hSlu7是正确选择3'剪接位点所必需的。在这里,我们通过生物信息学和突变分析确定了hSlu7蛋白的三个功能结构域,它们在其亚细胞定位中具有不同的作用:一个核定位信号、一个锌指基序和一个富含赖氨酸的区域。锌指基序以一种独特的功能结构嵌入核定位信号中,这对于hSlu7进入细胞核不是必需的,而是为了将hSlu7维持在细胞核内,防止其通过染色体区域维持1途径穿梭回细胞质。因此,hSlu7的锌指基序通过核质敏感的穿梭平衡决定了蛋白质的细胞定位。总之,这表明锌依赖性核质穿梭可能是hSlu7蛋白水平在细胞核内受到调控的可能分子基础。

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