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首页> 外文期刊>Scientific reports. >Human DNA-Damage-Inducible 2 Protein Is Structurally and Functionally Distinct from Its Yeast Ortholog
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Human DNA-Damage-Inducible 2 Protein Is Structurally and Functionally Distinct from Its Yeast Ortholog

机译:人体DNA损伤诱导型2蛋白在结构上和功能上与其酵母直脑不同

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Although Ddi1-like proteins are conserved among eukaryotes, their biological functions remain poorly characterized. Yeast Ddi1 has been implicated in cell cycle regulation, DNA-damage response, and exocytosis. By virtue of its ubiquitin-like (UBL) and ubiquitin-associated (UBA) domains, it has been proposed to serve as a proteasomal shuttle factor. All Ddi1-like family members also contain a highly conserved retroviral protease-like (RVP) domain with unknown substrate specificity. While the structure and biological function of yeast Ddi1 have been investigated, no such analysis is available for the human homologs. To address this, we solved the 3D structures of the human Ddi2 UBL and RVP domains and identified a new helical domain that extends on either side of the RVP dimer. While Ddi1-like proteins from all vertebrates lack a UBA domain, we identify a novel ubiquitin-interacting motif (UIM) located at the C-terminus of the protein. The UIM showed a weak yet specific affinity towards ubiquitin, as did the Ddi2 UBL domain. However, the full-length Ddi2 protein is unable to bind to di-ubiquitin chains. While proteomic analysis revealed no activity, implying that the protease requires other factors for activation, our structural characterization of all domains of human Ddi2 sets the stage for further characterization.
机译:虽然DDI1样蛋白在真核生物中被保守,但它们的生物学功能仍然很差。酵母DDI1涉及细胞周期调节,DNA损伤反应和卵尿量。凭借其泛素状的(UBL)和泛素相关的(UBA)结构域,已经提出作为蛋白酶体穿梭因子。所有DDI1的家庭成员还含有高度保守的逆转录病毒蛋白酶样(RVP)域,具有未知的底物特异性。虽然已经研究了酵母DDI1的结构和生物学功能,但是人类同源物没有使用这种分析。为了解决这个问题,我们解决了人DDI2 UBL和RVP域的3D结构,并识别了在RVP二聚体的任一侧延伸的新螺旋域。虽然来自所有脊椎动物的DDI1样蛋白缺乏UBA结构域,但我们鉴定位于蛋白质的C-末端的泛素相互作用的基序(UIM)。 UIM向遍毒蛋白表现出弱且特异性的亲和力,如DDI2 UBL结构域一样。然而,全长DDI2蛋白不能与二泛素链结合。虽然蛋白质组学分析没有揭示任何活动,但暗示蛋白酶需要其他因素进行活化,但我们对人DDI2的所有结构域的结构表征设定了进一步表征的阶段。

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