Department of Integrative Structural and Computational Biology, The Scripps Research Institute, La Jolla, CA, 92037, USA.
Department of Molecular Medicine, The Scripps Research Institute, La Jolla, CA, 92037, USA.
Nat Commun. 2018 Mar 28;9(1):1264. doi: 10.1038/s41467-018-03663-5.
The hemagglutinin (HA) receptor-binding site (RBS) in human influenza A viruses is critical for attachment to host cells, which imposes a functional constraint on its natural evolution. On the other hand, being part of the major antigenic sites, the HA RBS of human H3N2 viruses needs to constantly mutate to evade the immune system. From large-scale mutagenesis experiments, we here show that several of the natural RBS substitutions become integrated into an extensive epistatic network that prevents substitution reversion. X-ray structural analysis reveals the mechanistic consequences as well as changes in the mode of receptor binding. Further studies are necessary to elucidate whether such entrenchment limits future options for immune escape or adversely affect long-term viral fitness.
人甲型流感病毒的血凝素 (HA) 受体结合位点 (RBS) 对于与宿主细胞的附着至关重要,这对其自然进化施加了功能限制。另一方面,作为主要抗原位点的一部分,人 H3N2 病毒的 HA RBS 需要不断突变以逃避免疫系统。通过大规模的诱变实验,我们在这里表明,几种天然的 RBS 取代会整合到一个广泛的上位性网络中,从而阻止取代的逆转。X 射线结构分析揭示了机制后果以及受体结合模式的变化。需要进一步的研究来阐明这种根深蒂固的情况是否限制了未来的免疫逃逸选择,或者是否对病毒的长期适应性产生不利影响。
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