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Mechanisms of antiviral resistance in influenza neuraminidase revealed by a mass spectrometry based phylonumerics approach

机译:基于质谱法揭示植物血型血氨基氨基酶的抗病抗性机制

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摘要

A mass based phylonumerics approach is shown to be able to investigate the origins of the emergence of antiviral resistance mutations in influenza neuraminidase through a global view of mutational trends. Frequent ancestral and descendant mutations that precede and follow the manifestation of antiviral resistance mutations are identified in N2 neuraminidase. The majority occur in the head region around the active site and drive hydrophilicity changes, primarily through the incorporation or loss of hydroxyl groups. These increase or reduce the accessibility of the site to the bulk solvent. The most frequent ancestral mutations that occur on at least two occasions are I/L307M, G/A414S/T, I312T, I/L307S, P386S and S367N; the latter introducing a glycosylation site. The most frequent descendant mutation, after incorporation of an antiviral resistance mutation, is D/E401G/A. Together with others observed, this restore the protein's hydrophobicity about the active site region that limits entry of a sialic acid or inhibitor molecule and reduces viral fitness. The results of this global in silico phylonumerics study demonstrate that evolutionary mechanisms and functionally linked or compensatory mutations, remote in the sequence or structure, can be identified and interrogated at a molecular level.
机译:基于质量的植物学方法,能够通过全球突变趋势的观点来研究流感神经氨酸酶中​​抗病毒抗性突变的出现的起源。在N 2神经氨酸酶中​​鉴定出常见的祖先和后代突变和后遵循抗病毒抗性突变的表现。大多数发生在主动部位周围的头部区域,并推动亲水性改变,主要通过掺入或丧失羟基。这些增加或降低现场的可达性到批量溶剂。在至少两次发生的最常见的祖先突变是I / L307M,G / A414S / T,I312T,I / L307S,P386S和S367N;后者引入糖基化位点。掺入抗病毒抗性突变后,最常见的后代突变是D / E401G / A.与其他人一起观察到,这恢复了蛋白质的疏水性关于限制唾液酸或抑制剂分子的进入并降低病毒性的活性位点区域。这种全局在硅局的研究结果表明,可以在分子水平上鉴定和询问序列或结构的进化机制和功能链接或补偿突变,遥控突变。

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