A protective bispecific antibody targets both Nipah virus surface glycoproteins and limits viral escape

Ariel Isaacs
Guillermo Valenzuela Nieto
Xinghai Zhang
Naphak Modhiran
Jennifer Barr
Nazia Thakur
Yu Shang Low
Rhys H. Parry
James B. Barnes
Ronald Jara
Johanna Himelreichs
Yanfeng Yao
Camila Deride
Barbara Barthou-Gatica
Constanza Salinas-Rebolledo
Ehrenfeld Pamela
Jun Jet Hen
Noah Hayes
Devina Paramitha
Mahali S. Morgan
Christopher L.D. McMillan
Martina L. Jones
Trent Munro
Alexander A. Khromykh
Patrick C. Reading
Paul R. Young
Keith Chappell
Yi Shi
Dalan Bailey
Glenn Marsh
Sandra Chiu
Alejandro Rojas-Fernandez
Daniel Watterson

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Abstract

Nipah virus (NiV) and Hendra virus (HeV) are highly pathogenic henipaviruses without approved human vaccines or therapies. Here, we report on a highly potent bispecific therapeutic that combines an anti-fusion (F) nanobody with an anti-receptor binding protein (RBP) antibody to deliver a dual-targeting biologic that is resistant to viral escape. We show that the nanobody, DS90, engages a unique, conserved site within prefusion F of NiV and HeV, and provides neutralization and complete protection from NiV disease. Bispecific engineering of DS90 with the anti-RBP mAb m102.4 results in neutralization, elimination of viral escape and superior protection from NiV disease compared to leading monovalent approaches. These findings carry implications for the development of cross-neutralizing immunotherapies that limit the emergence of henipaviral escape mutants.

Version published to 10.1101/2025.03.11.642517v1 on bioRxiv
Mar 12, 2025

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