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Structural modeling of ataxin-3 reveals distant homology to adaptins.

机译:ataxin-3的结构建模揭示了与adaptins的远距离同源性。

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Spinocerebellar ataxia type 3 (SCA3) is a polyglutamine disorder caused by a CAG repeat expansion in the coding region of a gene encoding ataxin-3, a protein of yet unknown function. Based on a comprehensive computational analysis, we propose a structural model and structure-based functions for ataxin-3. Our predictive strategy comprises the compilation of multiple sequence and structure alignments of carefully selected proteins related to ataxin-3. These alignments are consistent with additional information on sequence motifs, secondary structure, and domain architectures. The application of complementary methods revealed the homology of ataxin-3 to ENTH and VHS domain proteins involved in membrane trafficking and regulatory adaptor functions. We modeled the structure of ataxin-3 using the adaptin AP180 as a template and assessed the reliability of the model by comparison with known sequence and structural features. We could further infer potential functions of ataxin-3 in agreement with known experimental data. Our database searches also identified an as yet uncharacterized family of proteins, which we named josephins because of their pronounced homology to the Josephin domain of ataxin-3.
机译:脊髓小脑性共济失调3型(SCA3)是由CAG重复扩增导致的,其编码功能未知的蛋白ataxin-3的基因的编码区引起的多谷氨酰胺紊乱。在全面的计算分析的基础上,我们提出了紫杉素3的结构模型和基于结构的功能。我们的预测策略包括精心选择的与紫杉醇3相关的蛋白质的多个序列和结构比对的汇编。这些比对与关于序列基序,二级结构和域结构的其他信息一致。互补方法的应用揭示了紫杉醇3与膜转运和调节衔接子功能所涉及的ENTH和VHS结构域蛋白的同源性。我们使用adaptin AP180作为模板对紫杉素-3的结构进行建模,并通过与已知序列和结构特征进行比较来评估模型的可靠性。我们可以根据已知的实验数据进一步推断紫杉素3的潜在功能。我们的数据库搜索还确定了一个尚未鉴定的蛋白质家族,我们将其命名为约瑟芬是因为它们与共济失调素3的约瑟芬域具有明显的同源性。

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