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Integration of structural dynamics and molecular evolution via protein interaction networks: a new era in genomic medicine

机译:通过蛋白质相互作用网络整合结构动力学和分子进化:基因组医学的新纪元

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摘要

Sequencing technologies are revealing many new non-synonymous single nucleotide variants (nsSNVs) in each personal exome. To assess their functional impacts, comparative genomics is frequently employed to predict if they are benign or not. However, evolutionary analysis alone is insufficient, because it misdiagnoses many disease-associated nsSNVs, such as those at positions involved in protein interfaces, and because evolutionary predictions do not provide mechanistic insights into functional change or loss. Structural analyses can aid in overcoming both of these problems by incorporating conformational dynamics and allostery in nSNV diagnosis. Finally, protein protein interaction networks using systems-level methodologies shed light onto disease etiology and pathogenesis. Bridging these network approaches with structurally resolved protein interactions and dynamics will advance genomic medicine.
机译:测序技术揭示了每个个人外显子组中许多新的非同义单核苷酸变体(nsSNV)。为了评估它们的功能影响,经常采用比较基因组学来预测它们是否良性。但是,仅靠进化分析是不够的,因为它会误诊许多与疾病相关的nsSNV,例如蛋白质界面所涉及的位置,并且因为进化预测无法提供对功能变化或丧失的机理见解。结构分析可以通过在nSNV诊断中结合构象动力学和变构来帮助克服这两个问题。最后,使用系统级方法的蛋白质相互作用网络阐明了疾病的病因和发病机理。将这些网络方法与结构解析的蛋白质相互作用和动力学联系起来,将推动基因组医学的发展。

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