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卷曲螺旋蛋白可与U7小核核糖核蛋白形成复合物。

Coilin can form a complex with the U7 small nuclear ribonucleoprotein.

作者信息

Bellini M, Gall J G

机构信息

Department of Embryology, Carnegie Institution, Baltimore, Maryland 21210, USA.

出版信息

Mol Biol Cell. 1998 Oct;9(10):2987-3001. doi: 10.1091/mbc.9.10.2987.

Abstract

Coiled bodies (CBs) in the amphibian oocyte nucleus are spherical structures up to 10 microm or more in diameter, much larger than their somatic counterparts, which rarely exceed 1 microm. Oocyte CBs may have smaller granules attached to their surface or embedded within them, which are identical in structure and composition to the many hundreds of B-snurposomes found free in the nucleoplasm. The matrix of the CBs contains the diagnostic protein p80-coilin, which is colocalized with the U7 small nuclear ribonucleoprotein (snRNP), whereas the attached and embedded B-snurposomes contain splicing snRNPs. A few of the 50-100 CBs in the oocyte nucleus are attached to lampbrush chromosomes at the histone gene loci. By coimmunoprecipitation we show that coilin and the U7 snRNP can form a weak but specific complex in the nucleoplasm, which is dependent on the special U7 Sm-binding site. Under the same conditions coilin does not associate with the U1 and U2 snRNPs. Coilin is a nucleic acid-binding protein, as shown by its interaction with single-stranded DNA and with poly r(U) and poly r(G). We suggest that an important function of coilin is to form a transient complex with the U7 snRNP and accompany it to the CBs. In the case of CBs attached to chromosomes at the histone gene loci, the U7 snRNP is thus brought close to the actual site of histone pre-mRNA transcription.

摘要

两栖类卵母细胞核中的卷曲小体(CBs)是直径达10微米或更大的球形结构,比其在体细胞中的对应物大得多,体细胞中的卷曲小体很少超过1微米。卵母细胞CBs的表面可能附着有较小的颗粒,或颗粒嵌入其中,这些颗粒在结构和组成上与在核质中游离的数百个B-核小核糖核蛋白体相同。CBs的基质含有诊断蛋白p80-卷曲螺旋蛋白,它与U7小核核糖核蛋白(snRNP)共定位,而附着和嵌入的B-核小核糖核蛋白体则含有剪接snRNPs。卵母细胞核中50-100个CBs中的一些附着在灯刷染色体的组蛋白基因位点上。通过免疫共沉淀,我们发现卷曲螺旋蛋白和U7 snRNP可以在核质中形成一个弱但特异的复合物,这依赖于特殊的U7 Sm结合位点。在相同条件下,卷曲螺旋蛋白不与U1和U2 snRNPs结合。卷曲螺旋蛋白是一种核酸结合蛋白,这可通过它与单链DNA、多聚r(U)和多聚r(G)的相互作用得以证明。我们认为卷曲螺旋蛋白的一个重要功能是与U7 snRNP形成一个瞬时复合物,并伴随它到达CBs。在组蛋白基因位点处附着于染色体的CBs的情况下,U7 snRNP因此被带到组蛋白前体mRNA转录的实际位点附近。

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