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一种保护性抗体鸡尾酒能够破坏拉沙病毒密集的糖基化外壳。

A cocktail of protective antibodies subverts the dense glycan shield of Lassa virus.

机构信息

Center for Infectious Disease and Vaccine Research, La Jolla Institute for Immunology, 9420 Athena Circle, La Jolla, CA 92037, USA.

Zalgen Labs LLC, 7495 New Horizon Way, Suite 120, Frederick, MD 21703, USA.

出版信息

Sci Transl Med. 2022 Oct 26;14(668):eabq0991. doi: 10.1126/scitranslmed.abq0991.

Abstract

Developing potent therapeutics and effective vaccines are the ultimate goals in controlling infectious diseases. Lassa virus (LASV), the causative pathogen of Lassa fever (LF), infects hundreds of thousands annually, but effective antivirals or vaccines against LASV infection are still lacking. Furthermore, neutralizing antibodies against LASV are rare. Here, we describe biochemical analyses and high-resolution cryo-electron microscopy structures of a therapeutic cocktail of three broadly protective antibodies that target the LASV glycoprotein complex (GPC), previously identified from survivors of multiple LASV infections. Structural and mechanistic analyses reveal compatible neutralizing epitopes and complementary neutralization mechanisms that offer high potency, broad range, and resistance to escape. These antibodies either circumvent or exploit specific glycans comprising the extensive glycan shield of GPC. Further, they require mammalian glycosylation, native GPC cleavage, and proper GPC trimerization. These findings guided engineering of a next-generation GPC antigen suitable for future neutralizing antibody and vaccine discovery. Together, these results explain protective mechanisms of rare, broad, and potent antibodies and identify a strategy for the rational design of therapeutic modalities against LF and related infectious diseases.

摘要

开发有效的治疗方法和疫苗是控制传染病的最终目标。拉沙病毒(LASV)是拉沙热(LF)的病原体,每年感染数十万人,但目前仍缺乏有效的 LASV 感染抗病毒药物或疫苗。此外,针对 LASV 的中和抗体也很少。在这里,我们描述了针对 LASV 糖蛋白复合物(GPC)的三种广泛保护抗体的治疗鸡尾酒的生化分析和高分辨率冷冻电子显微镜结构,这些抗体是从前多次 LASV 感染幸存者中鉴定出来的。结构和机制分析揭示了兼容的中和表位和互补的中和机制,具有高效力、广谱性和抗逃逸能力。这些抗体要么规避或利用包含 GPC 广泛糖基化的特定糖基。此外,它们需要哺乳动物糖基化、天然 GPC 切割和适当的 GPC 三聚体化。这些发现指导了下一代 GPC 抗原的工程设计,适用于未来中和抗体和疫苗的发现。总之,这些结果解释了罕见、广泛和有效的抗体的保护机制,并确定了针对 LF 和相关传染病的合理治疗方法设计策略。

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