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首页> 外文期刊>Nucleic Acids Research >Structural and biochemical studies of SLIP1-SLBP identify DBP5 and eIF3g as SLIP1-binding proteins
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Structural and biochemical studies of SLIP1-SLBP identify DBP5 and eIF3g as SLIP1-binding proteins

机译:SLIP1-SLBP的结构和生化研究确定DBP5和eIF3g为SLIP1结合蛋白

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摘要

In metazoans, replication-dependent histone mRNAs end in a stem-loop structure instead of the poly(A) tail characteristic of all other mature mRNAs. This specialized 3' end is bound by stem-loop binding protein (SLBP), a protein that participates in the nuclear export and translation of histone mRNAs. The translational activity of SLBP is mediated by interaction with SLIP1, a middle domain of initiation factor 4G (MIF4G)-like protein that connects to translation initiation. We determined the 2.5 angstrom resolution crystal structure of zebrafish SLIP1 bound to the translation-activation domain of SLBP and identified the determinants of the recognition. We discovered a SLIP1-binding motif (SBM) in two additional proteins: the translation initiation factor eIF3g and the mRNA-export factor DBP5. We confirmed the binding of SLIP1 to DBP5 and eIF3g by pull-down assays and determined the 3.25 angstrom resolution structure of SLIP1 bound to the DBP5 SBM. The SBM-binding and homodimerization residues of SLIP1 are conserved in the MIF4G domain of CBP80/20-dependent translation initiation factor (CTIF). The results suggest how the SLIP1 homodimer or a SLIP1-CTIF heterodimer can function as platforms to bridge SLBP with SBM-containing proteins involved in different steps of mRNA metabolism.
机译:在后生动物中,复制依赖的组蛋白mRNA终止于茎环结构,而不是所有其他成熟mRNA的poly(A)尾巴特征。这个专门的3'末端与茎环结合蛋白(SLBP)结合,该蛋白参与组蛋白mRNA的核输出和翻译。 SLBP的翻译活性是通过与SLIP1相互作用介导的,SLIP1是连接翻译起始的起始因子4G(MIF4G)样蛋白的中间结构域。我们确定了与SLBP的翻译激活域结合的斑马鱼SLIP1的2.5埃分辨率晶体结构,并确定了识别的决定因素。我们在另外两个蛋白质中发现了SLIP1结合基序(SBM):翻译起始因子eIF3g和mRNA出口因子DBP5。我们通过下拉测定法确认了SLIP1与DBP5和eIF3g的结合,并确定了与DBP5 SBM结合的SLIP1的3.25埃分辨率结构。 SLIP1的SBM结合和均二聚残基在CBP80 / 20依赖性翻译起始因子(CTIF)的MIF4G域中保守。结果表明,SLIP1同型二聚体或SLIP1-CTIF异二聚体如何充当平台,将SLBP与参与mRNA代谢不同步骤的含SBM蛋白质桥接。

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