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LRP130是一种单链DNA/RNA结合蛋白,定位于核外膜和内质网膜,并在体内与mRNA相互作用。

LRP130, a single-stranded DNA/RNA-binding protein, localizes at the outer nuclear and endoplasmic reticulum membrane, and interacts with mRNA in vivo.

作者信息

Tsuchiya Naoto, Fukuda Hirokazu, Nakashima Katsuhiko, Nagao Minako, Sugimura Takashi, Nakagama Hitoshi

机构信息

Biochemistry Division, National Cancer Center Research Institute, 5-1-1 Tsukiji Chuo-ku, Tokyo 104-0045, Japan.

出版信息

Biochem Biophys Res Commun. 2004 May 7;317(3):736-43. doi: 10.1016/j.bbrc.2004.03.103.

Abstract

LRP130 (also known as a LRPPRC) is an RNA and single-stranded DNA-binding protein, and recently identified as a candidate gene responsible for the Leigh syndrome, a French-Canadian type cytochrome c oxidase deficiency. However, the biological function of LRP130 still remains largely unresolved. In the present study, we found that the C-terminal half of the mouse LRP130 located within a 120 amino acid sequence (a.a. 845-964) binds to synthetic RNA homopolymers, poly(G), poly(U), and poly(C), as well as r(CUGCC)(6). Assessment of the subcellular localization indicated both nuclear/endoplasmic reticulum (ER) and mitochondrial fractions to be positive. To further analyze the subcellular localization of LRP130, a nuclear/ER fraction was fractionated into the nucleoplasm (NP) and nuclear envelope (NE)/ER, and the latter was further separated into outer nuclear membrane (ONM)/ER and inner nuclear membrane (INM) by treatment with Triton X-100. LRP130 was detectable in all three fractions, and the distribution pattern was in good accordance with that known for ONM/ER proteins. Interestingly, immunostaining of HeLa cells demonstrated nuclear rim staining of LRP130, specifically at the outside of the NE and also at ER, and association of LRP130 with poly(A)(+) RNA was restricted only to the ONM/ER fraction. Overexpression of full-length mouse LRP130 fused with EGFP resulted in nuclear accumulation of poly(A)(+) RNA in HeLa cells. Taking all these results together, it is suggested that LRP130, a novel type of RNA-binding protein, associates with mRNA/mRNP complexes at the outside of NE and ER, and plays a role in control of mRNA metabolisms.

摘要

LRP130(也称为LRPPRC)是一种RNA和单链DNA结合蛋白,最近被确定为导致法裔加拿大人型细胞色素c氧化酶缺乏的 Leigh 综合征的候选基因。然而,LRP130的生物学功能在很大程度上仍未得到解决。在本研究中,我们发现小鼠LRP130位于120个氨基酸序列(第845 - 964位氨基酸)内的C末端一半与合成RNA同聚物、聚(G)、聚(U)和聚(C)以及r(CUGCC)(6)结合。亚细胞定位评估表明核/内质网(ER)和线粒体部分均呈阳性。为了进一步分析LRP130的亚细胞定位,将核/ER部分分离为核质(NP)和核膜(NE)/ER,后者通过用Triton X - 100处理进一步分离为外核膜(ONM)/ER和内核膜(INM)。在所有这三个部分中都可检测到LRP130,并且分布模式与已知的ONM/ER蛋白的分布模式非常一致。有趣的是,HeLa细胞的免疫染色显示LRP130的核边缘染色,特别是在NE的外侧以及ER处,并且LRP130与聚(A)(+) RNA的关联仅限于ONM/ER部分。与EGFP融合的全长小鼠LRP130的过表达导致HeLa细胞中聚(A)(+) RNA的核积累。综合所有这些结果,表明LRP130是一种新型的RNA结合蛋白,在NE和ER外侧与mRNA/mRNP复合物相关联,并在mRNA代谢控制中发挥作用。

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