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Human SAP18 mediates assembly of a splicing regulatory multiprotein complex via its ubiquitin-like fold

机译:人类SAP18通过其遍在蛋白样折叠介导剪接调节性多蛋白复合物的组装

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摘要

RNPS1, Acinus, and SAP18 form the apoptosis- and splicing-associated protein (ASAP) complex, which is also part of the exon junction complex. Whereas RNPS1 was originally identified as a general activator of mRNA processing, all three proteins have been found within functional spliceosomes. Both RNPS1 and Acinus contain typical motifs of splicing regulatory proteins including arginine/serine-rich domains. Due to the absence of such structural features, however, a function of SAP18 in splicing regulation is completely unknown. Here we have investigated splicing regulatory activities of the ASAP components. Whereas a full-length Acinus isoform displayed only limited splicing regulatory activity, both RNPS1 and, surprisingly, SAP18 strongly modulated splicing regulation. Detailed mutational analysis and three-dimensional modeling data revealed that the ubiquitin-like fold of SAP18 was required for efficient splicing regulatory activity. Coimmunoprecipitation and immunofluorescence experiments demonstrated that SAP18 assembles a nuclear speckle-localized splicing regulatory multiprotein complex including RNPS1 and Acinus via its ubiquitin-like fold. Our results therefore suggest a novel function of SAP18 in splicing regulation.
机译:RNPS1,Acinus和SAP18形成凋亡和剪接相关蛋白(ASAP)复合物,它也是外显子连接复合物的一部分。 RNPS1最初被确定为mRNA加工的一般激活因子,而在功能性剪接体中发现了这三种蛋白。 RNPS1和Acinus均包含剪接调节蛋白(包括精氨酸/富含丝氨酸的域)的典型基序。然而,由于缺乏这种结构特征,SAP18在剪接调控中的功能是完全未知的。在这里,我们研究了ASAP组件的拼接监管活动。全长牛粪亚型仅显示有限的剪接调节活性,而RNPS1和令人惊讶的是SAP18均强烈调节剪接调节。详细的突变分析和三维建模数据显示,SAP18的泛素样折叠是有效剪接调控活性所必需的。免疫共沉淀和免疫荧光实验表明,SAP18通过其遍在蛋白样折叠组装了一个包含核斑点定位的剪接调控多蛋白复合物,包括RNPS1和Acinus。因此,我们的结果表明了SAP18在剪接调控中的新功能。

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