Measles virus (MeV) presents a public health threat that is escalating as vaccine coverage in the general population declines and as populations of immunocompromised individuals, who cannot be vaccinated, increase. There are no approved therapeutics for MeV. Neutralizing antibodies targeting viral fusion are one potential therapeutic approach but have not yet been structurally characterized or advanced to clinical use. We present cryo-electron microscopy (cryo-EM) structures of prefusion F alone [2.1-angstrom (Ã ) resolution], F complexed with a fusion-inhibitory peptide (2.3-Ã resolution), F complexed with the neutralizing and protective monoclonal antibody (mAb) 77 (2.6-Ã resolution), and an additional structure of postfusion F (2.7-Ã resolution). In vitro assays and examination of additional EM classes show that mAb 77 binds prefusion F, arrests F in an intermediate state, and prevents transition to the postfusion conformation. These structures shed light on antibody-mediated neutralization that involves arrest of fusion proteins in an intermediate state.
A neutralizing antibody prevents postfusion transition of measles virus fusion protein.
中和抗体可阻止麻疹病毒融合蛋白的融合后转变
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作者:Zyla Dawid S, Della Marca Roberta, Niemeyer Gele, Zipursky Gillian, Stearns Kyle, Leedale Cameron, Sobolik Elizabeth B, Callaway Heather M, Hariharan Chitra, Peng Weiwei, Parekh Diptiben, Marcink Tara C, Diaz Avalos Ruben, Horvat Branka, Mathieu Cyrille, Snijder Joost, Greninger Alexander L, Hastie Kathryn M, Niewiesk Stefan, Moscona Anne, Porotto Matteo, Saphire Erica Ollmann
| 期刊: | Science | 影响因子: | 45.800 |
| 时间: | 2024 | 起止号: | 2024 Jun 28; 384(6703):eadm8693 |
| doi: | 10.1126/science.adm8693 | 研究方向: | 免疫/内分泌 |
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