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PROTEIN INTERACTIONS AND DISEASE PHENOTYPES IN THE ABC TRANSPORTER SUPERFAMILY

机译:ABC转运蛋白的蛋白质相互作用和疾病表型超家族

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摘要

ABC transporter proteins couple the energy of ATP binding and hydrolysis to substrate transport across a membrane. In humans, clinical studies have implicated mutations in 19 of the 48 known ABC transporters in diseases such as cystic fibrosis and adrenoleukodystrophy. Although divergent in sequence space, the overall topology of these proteins, consisting of two transmembrane domains and two ATP-binding cassettes, is likely to be conserved across diverse organisms. We examine known intra-transporter domain interfaces using crystallographic structures of isolated and complexed domains in ABC transporter proteins and find that the nucleotide binding domain interfaces are better conserved than interfaces at the transmembrane domains. We then apply this analysis to identify known disease-associated point and deletion mutants for which disruption of domain-domain interfaces might indicate the mechanism of disease. Finally, we suggest a possible interaction site based on conservation of sequence and disease-association of point mutants.
机译:ABC转运蛋白蛋白将ATP结合和水解的能量耦合到膜上的底物输送。在人类中,临床研究在诸如囊性纤维化和肾上腺般的疾病中的48名已知的ABC转运蛋白中有含有含有的突变。尽管在序列空间中发散,但是由两个跨膜结构域和两个ATP结合盒组成的这些蛋白质的整体拓扑可能在不同的生物体上被保守。我们使用ABC转运蛋白中的分离和复合结构域的结晶结构检查已知的转运机域界面,并发现核苷酸结合域界面比跨膜结构域的界面更好地保守。然后,我们应用该分析以鉴定已知的疾病相关点和缺失突变体,其中域域界面的破坏可能表明疾病的机制。最后,我们建议一种基于序列和疾病关联的序列和疾病关联的可能的相互作用。

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