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首页> 外文期刊>FEBS Letters >The solution structure of the viral binding domain of Tva, the cellular receptor for subgroup A avian leukosis and sarcoma virus1
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The solution structure of the viral binding domain of Tva, the cellular receptor for subgroup A avian leukosis and sarcoma virus1

机译:Tva病毒结合结构域的溶液结构,A亚群禽白血病和肉瘤病毒的细胞受体1

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>The cellular receptor for subgroup A avian leukosis and sarcoma virus (ALSV-A) is Tva, which contains a motif related to repeats in the low density lipoprotein receptor (LDLR) ligand binding repeat (LBr) and which is necessary for viral entry. As observed with LBr repeats of LDLR, the 47 residue LBr domain of Tva (sTva47) requires calcium during oxidative folding to form the correct disulfide bonds, and calcium enhances the structure of correctly oxidized sTva47, as well as its ability to bind the viral envelope protein (Env). However, solution nuclear magnetic resonance studies indicate that, even in the presence of excess calcium, sTva47 exists in an ensemble of conformations. Nonetheless, as reported here, the structure of the predominant sTva47 solution conformer closely resembles that of other LBr repeats, with identical S–S binding topology and octahedral calcium coordination. The location of W48 and other critical residues on the surface suggests a region of the molecule necessary for Env binding and to mediate post-binding events important for ALSV-A cell entry.
机译:>禽流感和肉瘤病毒亚组(ALSV-A)的细胞受体是Tva,它包含与低密度脂蛋白受体(LDLR)配体结合重复序列(LBr)中的重复序列相关的基序,并且对于病毒而言是必需的条目。正如LDLR的LBr重复序列所观察到的那样,Tva的47个残基LBr结构域(sTva47)在氧化折叠过程中需要钙以形成正确的二硫键,并且钙增强了正确氧化的sTva47的结构及其结合病毒包膜的能力蛋白质(Env)。但是,溶液核磁共振研究表明,即使存在过量的钙,sTva47仍以构象形式存在。但是,如此处报道,主要的sTva47溶液构象异构体的结构与其他LBr重复序列非常相似,具有相同的S–S结合拓扑和八面体钙配位。 W48和其他关键残基在表面上的位置暗示了Env结合并介导对ALSV-A细胞进入重要的结合后事件所必需的分子区域。

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