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首页> 外文期刊>Journal of Molecular Biology >Molecular determinants of PAM2 recognition by the MLLE domain of poly(A)-binding protein.
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Molecular determinants of PAM2 recognition by the MLLE domain of poly(A)-binding protein.

机译:分子决定因素通过poly(A)结合蛋白的MLLE域识别PAM2。

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摘要

MLLE (previously known as PABC) is a peptide-binding domain that is found in poly(A)-binding protein (PABP) and EDD (E3 isolated by differential display), a HECT E3 ubiquitin ligase also known as HYD (hyperplastic discs tumor suppressor) or UBR5. The MLLE domain from PABP recruits various regulatory proteins and translation factors to poly(A) mRNAs through binding of a conserved 12 amino acid peptide motif called PAM2 (for PABP-interacting motif 2). Here, we determined crystal structures of the MLLE domain from PABP alone and in complex with PAM2 peptides from PABP-interacting protein 2. The structures provide a detailed view of hydrophobic determinants of the MLLE binding coded by PAM2 positions 3, 5, 7, 10, and 12 and reveal novel intermolecular polar contacts. In particular, the side chain of the invariant MLLE residue K580 forms hydrogen bonds with the backbone of PAM2 residues 5 and 7. The structures also show that peptide residues outside of the conserved PAM2 motif contribute to binding. Altogether, the structures provide a significant advance in understanding the molecular basis for the binding of PABP by PAM2-containing proteins involved in translational control, mRNA deadenylation, and other cellular processes.
机译:MLLE(以前称为PABC)是一种多肽结合域,存在于poly(A)结合蛋白(PABP)和EDD(通过差异展示分离的E3)中,HECT E3泛素连接酶也称为HYD(增生性椎间盘肿瘤抑制器)或UBR5。 PABP的MLLE结构域通过结合称为PAM2的保守12个氨基酸肽基序(对于与PABP相互作用的基序2),将各种调节蛋白和翻译因子募集到poly(A)mRNA。在这里,我们确定了来自PABP的MLLE结构域的晶体结构,并与来自PABP相互作用蛋白2的PAM2肽复合。该结构提供了由PAM2位置3、5、7、10编码的MLLE结合的疏水决定簇的详细视图。和12,揭示了新颖的分子间极性接触。特别地,不变的MLLE残基K580的侧链与PAM2残基5和7的主链形成氢键。该结构还表明保守的PAM2基序之外的肽残基有助于结合。总之,该结构在理解分子翻译基础方面提供了重大进展,该分子基础是与翻译控制,mRNA腺苷酸化和其他细胞过程有关的含PAM2的蛋白质与PABP结合的基础。

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