Fully human single-domain antibody targeting a highly conserved cryptic epitope on the Nipah virus G protein

Author:

Ying Tianlei1ORCID,Wang Yulu2,Sun Yifang3,Shen Zhaoling1,Wang Cong1,Qian Jun1,Mao Qiyu3,Wang Yajie1,Song Wenping1,Kong Yu1,Zhan Changyou1ORCID,Chen Zhenguo1ORCID,Dimitrov Dimiter4,Yang Zhenlin1,Jiang Shibo1ORCID,Wu Fan1,Lu Lu1ORCID,Sun Lei1ORCID,Wu Yanling1

Affiliation:

1. Fudan University

2. Shanghai Medical College of Fudan University

3. Shanghai Fifth People's Hospital, Fudan University, and Shanghai Key Laboratory of Medical Epigenetics, International Co-laboratory of Medical Epigenetics and Metabolism (Ministry of Science and Tec

4. University of Pittsburgh

Abstract

Abstract

Nipah virus infection, one of the top priority diseases recognized by the World Health Organization, underscores the urgent need to develop effective countermeasures against potential epidemics and pandemics. Here, we identified a fully human single-domain antibody that targets a highly conserved cryptic epitope situated at the dimeric interface of the Nipah virus G protein (receptor binding protein, RBP), as elucidated through structures by high-resolution cryo-electron microscopy (cryo-EM). This unique binding mode disrupts the tetramerization of the G protein stalk domain, consequently obstructing the activation of the F protein and inhibiting viral membrane fusion. Furthermore, our investigations revealed that this compact antibody displays enhanced permeability across the blood-brain barrier (BBB) and demonstrates superior efficacy in eliminating pseudovirus within the brain in a murine model of Nipah virus infection, particularly compared to the well-characterized antibody m102.4 in an IgG1 format. Consequently, this single-domain antibody holds promise as a therapeutic candidate to prevent Nipah virus infections and has potential implications for vaccine development.

Publisher

Springer Science and Business Media LLC

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