Inhaled “Muco‐Trapping” Monoclonal Antibody Effectively Treats Established Respiratory Syncytial Virus (RSV) Infections

Author:

McSweeney Morgan D.1ORCID,Alnajjar Sarhad2,Schaefer Alison M.3,Richardson Zach1,Wolf Whitney3,Stewart Ian4,Sriboonyapirat Pun5,McCallen Justin3,Farmer Ellen1,Nzati Bernadette1,Lord Sam1,Farrer Brian1,Moench Thomas R.1,Kumar Priya A.67,Arora Harendra8,Pickles Raymond J.9,Hickey Anthony J.4,Ackermann Mark10,Lai Samuel K.139ORCID

Affiliation:

1. Inhalon Biopharma Research Triangle Park NC 27707 USA

2. Department of Comparative Biomedical Sciences, School of Veterinary Medicine, Faculty of Health and Medical Sciences University of Surrey Guildford GU2 7AL UK

3. Division of Pharmacoengineering and Molecular Pharmaceutics, Eshelman School of Pharmacy University of North Carolina‐Chapel Hill Chapel Hill NC 27599 USA

4. RTI International Research Triangle Park NC 27709 USA

5. Oregon State University Corvallis Oregon 97331 USA

6. Department of Anesthesiology, School of Medicine University of North Carolina Chapel Hill NC 27599 USA

7. Outcomes Research Consortium Cleveland OH 44195 USA

8. Department of Anesthesiology University of Mississippi Medical Center Jackson MS 39216 USA

9. Department of Microbiology & Immunology, School of Medicine University of North Carolina at Chapel Hill Chapel Hill NC 27599 USA

10. USDA/ARS‐National Animal Disease Center Ames IA 50010 USA

Abstract

AbstractRespiratory syncytial virus (RSV) causes substantial morbidity and mortality in infants, the immunocompromised, and the elderly. RSV infects the airway epithelium via the apical membrane and almost exclusively sheds progeny virions back into the airway mucus (AM), making RSV difficult to target by systemically administered therapies. An inhalable “muco‐trapping” variant of motavizumab (Mota‐MT), a potent neutralizing mAb against RSV F is engineered. Mota‐MT traps RSV in AM via polyvalent Fc‐mucin bonds, reducing the fraction of fast‐moving RSV particles in both fresh pediatric and adult AM by ≈20–30‐fold in a Fc‐glycan dependent manner, and facilitates clearance from the airways of mice within minutes. Intranasal dosing of Mota‐MT eliminated viral load in cotton rats within 2 days. Daily nebulized delivery of Mota‐MT to RSV‐infected neonatal lambs, beginning 3 days after infection when viral load is at its maximum, led to a 10 000‐fold and 100 000‐fold reduction in viral load in bronchoalveolar lavage and lung tissues relative to placebo control, respectively. Mota‐MT‐treated lambs exhibited reduced bronchiolitis, neutrophil infiltration, and airway remodeling than lambs receiving placebo or intramuscular palivizumab. The findings underscore inhaled delivery of muco‐trapping mAbs as a promising strategy for the treatment of RSV and other acute respiratory infections.

Funder

National Institutes of Health

David and Lucile Packard Foundation

National Science Foundation

Publisher

Wiley

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