An Attachment Glycoprotein Nanoparticle Elicits Broadly Neutralizing Antibodies and Protects Against Lethal Nipah Virus Infection

Overview

Journal NPJ Vaccines

Date 2024 Aug 31

PMID 39217188

Authors

Dan Zhou

Rao Cheng

Yanfeng Yao

Gan Zhang

Xin Li

Bingjie Wang

Yong Wang

Feiyang Yu

Shangyu Yang

Hang Liu

Ge Gao

Yun Peng

Miaoyu Chen

Zengqin Deng

Haiyan Zhao

Affiliations

Soon will be listed here.

Abstract

Nipah virus (NiV) is a zoonotic emergent paramyxovirus that can cause severe encephalitis and respiratory infections in humans, with a high fatality rate ranging from 40% to 75%. Currently, there are no approved human vaccines or antiviral drugs against NiV. Here, we designed a ferritin-based self-assembling nanoparticle displaying the NiV G head domain on the surface (NiV G-ferritin) and assessed immune responses elicited by the soluble NiV G head domain (NiV sG) or NiV G-ferritin. Immunization with NiV G-ferritin or NiV sG conferred complete protection against lethal NiV challenge without detection of viral RNA in Syrian golden hamsters. Compared to NiV sG, NiV G-ferritin induced significantly faster, broader, and higher serum neutralizing responses against three pathogenic henipaviruses (NiV-Malaysia, NiV-Bangladesh, and Hendra virus). Moreover, NiV G-ferritin induced a durable neutralizing immunity in mice as antisera potently inhibited NiV infection even after six months of the third immunization. Additionally, we isolated a panel of 27 NiV G-binding monoclonal antibodies (mAbs) from NiV G-ferritin immunized mice and found that these mAbs targeted four distinct antigenic sites on NiV G head domain with two sites that have not been defined previously. Notably, 25 isolated mAbs have potent neutralizing activity with 50% inhibitory concentrations less than 10 ng/mL against NiV pseudovirus. Collectively, these findings provide new insights into the immunogenicity of NiV G protein and reveal that NiV G-ferritin is a safe and highly effective vaccine candidate against Nipah virus infection.

Citing Articles

Cross-protectivity of henipavirus soluble glycoprotein in an model of Nipah virus disease.

Findlay-Wilson S, Thakur N, Crossley L, Easterbrook L, Salguero F, Ruedas-Torres I Front Immunol. 2025; 16:1517244.

PMID: 40078997 PMC: 11896980. DOI: 10.3389/fimmu.2025.1517244.

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