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Ubiquitin binding by a variant Jab1/MPN domain in the essential pre-mRNA splicing factor Prp8p

机译:泛素结合必需的前mRNA剪接因子Prp8p中的一个Jab1 / MPN变异域

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摘要

The U1, U2, U4/U6, and U5 small nuclear ribonucleoproteins (snRNPs) are components of the spliceosome, which catalyzes pre-mRNA splicing. One of the largest and the most highly conserved proteins in the spliceosome is Prp8p, a component of the U5 snRNP. Despite its size and conservation, very few motifs have been identified that suggest specific biochemical functions. A variant of the Jab1/MPN domain found in a class of deubiquitinating enzymes is present near the C terminus of Prp8p. Ubiquitination regulates a broad range of cellular pathways, and its functions generally require ubiquitin recognition by one or more ubiquitin-binding domains (UBDs). No precise role for ubiquitin has been defined in the pre-mRNA splicing pathway, and no known UBDs have been found within splicing proteins. Here we show that a Prp8p fragment containing the Jab1/MPN domain binds directly to ubiquitin with an affinity comparable to other known UBDs. Several mutations within this domain that compromise splicing also reduce interaction of the fragment with ubiquitin-Sepharose. Our results define a new UBD and suggest functional links between ubiquitin and the pre-mRNA splicing machinery.
机译:U1,U2,U4 / U6和U5小核糖核糖核蛋白(snRNP)是剪接体的组成部分,可催化mRNA的剪接。剪接体中最大和最高度保守的蛋白质之一是Prp8p,它是U5 snRNP的一个组成部分。尽管其大小和保守性,很少被发现暗示特定的生化功能的图案。在一类去泛素化酶中发现的Jab1 / MPN域的变体位于Prp8p的C末端附近。泛素化调节广泛的细胞途径,其功能通常需要一个或多个泛素结合域(UBD)的泛素识别。在mRNA的前剪接途径中尚未确定泛素的确切作用,并且在剪接蛋白中未发现已知的UBD。在这里,我们显示包含Jab1 / MPN域的Prp8p片段直接结合到遍在蛋白上,其亲和力可与其他已知UBD媲美。该结构域内危及剪接的几个突变也减少了该片段与泛素-琼脂糖的相互作用。我们的结果定义了一种新的UBD,并提示泛素和mRNA前剪接机制之间的功能联系。

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