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Network of coordinated substitutions in the Hepatitis B virus polymerase

机译:乙型肝炎病毒聚合酶中的协调取代网络

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We analyzed coordinated variation among amino acid sites in 370 HBV polymerase sequences using Bayesian networks. Among the HBV polymerase domains the spacer domain separating terminal protein from the reverse-transcriptase domain, showed the highest network centrality. Coordinated substitutions preserve the hydrophobicity and charge of Spacer. Maximum likelihood estimates of codon selection showed that Spacer contains the highest number of positively selected sites. Identification of 67% of the domain lacking an ordered structure suggests that Spacer belongs to the class of intrinsically unstructured domains and proteins whose crucial functional role in the regulation of transcription, translation and cellular signal transduction has only recently been recognized. Spacer plays a central role in the epistatic network associating substitutions across the HBV genome, including those conferring viral virulence, drug resistance and vaccine escape.
机译:我们使用贝叶斯网络分析了370 HBV聚合酶序列中氨基酸位点之间的协调变异。在HBV聚合酶结构域中,将末端蛋白与逆转录酶结构域隔开的间隔子结构域显示出最高的网络中心性。配位取代保留了间隔基的疏水性和电荷。密码子选择的最大似然估计表明,Spacer包含最多数量的正向选择位点。 67%的结构域缺乏有序结构的鉴定表明,Spacer属于内在非结构化结构域和蛋白质,其在转录,翻译和细胞信号转导的调节中的关键功能仅在最近才被认识到。间隔子在与整个HBV基因组相关的取代相关的上位网络中起着核心作用,包括那些赋予病毒毒力,耐药性和疫苗逃逸的取代。

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