Department of Integrative Structural and Computational Biology, The Scripps Research Institute, La Jolla, California, United States of America.
Department of Pathology, Microbiology and Immunology, Vanderbilt University School of Medicine, Nashville, Tennessee, United States of America.
PLoS Biol. 2019 Feb 4;17(2):e3000139. doi: 10.1371/journal.pbio.3000139. eCollection 2019 Feb.
Seasonal influenza virus infections can cause significant morbidity and mortality, but the threat from the emergence of a new pandemic influenza strain might have potentially even more devastating consequences. As such, there is intense interest in isolating and characterizing potent neutralizing antibodies that target the hemagglutinin (HA) viral surface glycoprotein. Here, we use cryo-electron microscopy (cryoEM) to decipher the mechanism of action of a potent HA head-directed monoclonal antibody (mAb) bound to an influenza H7 HA. The epitope of the antibody is not solvent accessible in the compact, prefusion conformation that typifies all HA structures to date. Instead, the antibody binds between HA head protomers to an epitope that must be partly or transiently exposed in the prefusion conformation. The "breathing" of the HA protomers is implied by the exposure of this epitope, which is consistent with metastability of class I fusion proteins. This structure likely therefore represents an early structural intermediate in the viral fusion process. Understanding the extent of transient exposure of conserved neutralizing epitopes also may lead to new opportunities to combat influenza that have not been appreciated previously.
季节性流感病毒感染可导致严重的发病率和死亡率,但新出现的大流行性流感毒株所带来的威胁可能具有更具破坏性的潜在后果。因此,人们强烈关注分离和鉴定针对血凝素 (HA) 病毒表面糖蛋白的有效中和抗体。在这里,我们使用冷冻电子显微镜 (cryoEM) 来阐明与流感 H7 HA 结合的强效 HA 头部定向单克隆抗体 (mAb) 的作用机制。该抗体的表位在迄今所有 HA 结构中典型的紧凑、预融合构象中不可溶。相反,抗体结合在 HA 头部三聚体之间,结合的表位在预融合构象中必须部分或暂时暴露。该表位的暴露暗示了 HA 三聚体的“呼吸”,这与 I 类融合蛋白的不稳定性一致。因此,该结构可能代表病毒融合过程中的早期结构中间体。了解保守中和表位的瞬时暴露程度也可能为以前未被重视的对抗流感的新机会提供途径。
