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IMP1 interacts with poly(A)-binding protein (PABP) and the autoregulatory translational control element of PABP-mRNA through the KHIII-IV domain

机译:IMP1通过KHIII-IV结构域与poly(A)结合蛋白(PABP)和PABP-mRNA的自调控翻译控制元件相互作用

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摘要

Repression of poly(A)-binding protein (PABP) mRNA translation involves the formation of a heterotrimeric ribonucleoprotein complex by the binding of PABP, insulin-like growth factor II mRNA binding protein-1 (IMP1) and the unr gene encoded polypeptide (UNR) to the adenine-rich autoregulatory sequence (ARS) located at the 5' untranslated region of the PABP-mRNA. In this report, we have further characterized the interaction between PABP and IMP1 with the ARS at the molecular level. The dissociation constants of PABP and IMP1 for binding to the ARS RNA were determined to be 2.3 nM and 5.9 nM, respectively. Both PABP and IMP1 interact with each other, regardless of the presence of the ARS, through the conserved C-terminal PABP-C and K-homology (KH) III-IV domains, respectively. Interaction of PABP with the ARS requires at least three out of its four RNA-binding domains, whereas KH III-IV domain of IMP1 is necessary and sufficient for binding to the ARS. In addition, the strongest binding site for both PABP and IMP1 on the ARS was determined to be within the 22 nucleotide-long CCCAAAAAAAUUUACAAAAAA sequence located at the 3' end of the ARS. Results of our analysis suggest that both protein.protein and protein.RNA interactions are involved in forming a stable ribonucleoprotein complex at the ARS of PABP mRNA.
机译:抑制poly(A)结合蛋白(PABP)mRNA翻译涉及通过PABP,胰岛素样生长因子II mRNA结合蛋白-1(IMP1)和unr基因编码的多肽(UNR)的结合形成异三聚核糖核蛋白复合物。 )到位于PABP-mRNA 5'非翻译区的富含腺嘌呤的自动调节序列(ARS)。在本报告中,我们在分子水平上进一步表征了PABP和IMP1与ARS之间的相互作用。与ARS RNA结合的PABP和IMP1的解离常数分别确定为2.3 nM和5.9 nM。无论是否存在ARS,PABP和IMP1都通过保守的C端PABP-C和K-同源(KH)III-IV域相互相互作用。 PABP与ARS的相互作用至少需要其四个RNA结合结构域中的三个,而IMP1的KH III-IV结构域对于结合ARS是必需的且足够的。此外,确定了ARS上PABP和IMP1的最强结合位点位于位于ARS 3'端的22个核苷酸长的CCCAAAAAAAUUUACAAAAAAAAA序列内。我们的分析结果表明,蛋白质,蛋白质和蛋白质,RNA相互作用都参与在PABP mRNA的ARS处形成稳定的核糖核蛋白复合物。

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