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Antigen-antibody interactions of influenza virus hemagglutinin revealed by the fragment molecular orbital calculation

机译:片段分子轨道计算揭示流感病毒血凝素的抗原-抗体相互作用

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Effective interactions between amino acid residues in antigen-antibody complex of influenza virus hemagglutinin (HA) protein can be evaluated in terms of the inter-fragment interaction energy (IFIE) analysis with the fragment molecular orbital (FMO) method, in which each fragment contains the side chain of corresponding amino acid residue. We have carried out the FMO-MP2 (second-order Moeller-Plesset) calculation for the complex of HA antigen and Fab antibody of influenza virus H3N2 A/Aichi/2/68 and obtained the IFIE values between each amino acid residue in HA and the whole antibody as the sums over the residues contained in the latter. Combining this IFIE data with experimental data for hemadsorptionactivity of HA mutants, we succeeded in theoretically explaining the mutations in HA observed after the emergence of influenza virus H3N2 A/Aichi/2/68 in an earlier study, except for those of THR83. in the present study, we employ an alternative way of fragment division in the FMO calculation at the carbonyl C site of the peptide bond instead of the C_α site used in the previous work, which provides revised IFIE values consistent with all the historical mutation data in the antigenic region E of HA including the case of THR83 in the present prediction scheme for probable mutations in HA.
机译:流感病毒血凝素(HA)蛋白抗原-抗体复合物中氨基酸残基之间的有效相互作用可以通过片段分子轨道(FMO)方法的片段间相互作用能(IFIE)分析来评估,其中每个片段均包含相应氨基酸残基的侧链。我们已经对流感病毒H3N2 A / Aichi / 2/68的HA抗原和Fab抗体的复合物进行了FMO-MP2(二阶Moeller-Plesset)计算,并获得了HA和完整抗体的总和为后者所含残基的总和。将IFIE数据与HA突变体的血液吸附活性实验数据相结合,我们在理论上成功地解释了在早期研究中,除了THR83突变外,在流感病毒H3N2 A / Aichi / 2/68出现后观察到的HA突变。在本研究中,我们在FMO计算中采用了另一种片段分割方法,即在肽键的羰基C位点而不是之前的工作中使用的C_α位点,该方法提供了与所有历史突变数据一致的IFIE值在HA的可能突变的本预测方案中,HA的抗原区域E包括THR83的情况。

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