Literature DB >> 31101672

A lipid-encapsulated mRNA encoding a potently neutralizing human monoclonal antibody protects against chikungunya infection.

Nurgun Kose1, Julie M Fox2, Gopal Sapparapu1,3, Robin Bombardi1, Rashika N Tennekoon4, A Dharshan de Silva4,5, Sayda M Elbashir6, Matthew A Theisen6, Elisabeth Humphris-Narayanan6, Giuseppe Ciaramella6, Sunny Himansu6, Michael S Diamond2,7, James E Crowe8,3,9.   

Abstract

Infection with chikungunya virus (CHIKV) causes an acute illness characterized by fever, rash, and arthralgia. However, CHIKV infection can sometimes progress to chronic arthritis or even lethal disease. CHIKV continues to cause substantial morbidity worldwide as its vector mosquitoes expand and spread. There are currently no approved vaccines or antiviral drugs available for the prevention or treatment of CHIKV. Although antibody therapy has shown promise in the prevention or treatment of CHIKV disease in preclinical models, challenges remain for implementing such therapies. Here, from the B cells of a survivor of natural CHIKV infection, we isolated ultrapotent neutralizing human monoclonal antibodies (mAbs) and encoded their sequences into mRNA molecules delivered by infusion. One human mAb, CHKV-24, was expressed to biologically significant levels in vivo after infusion of mRNAs in lipid nanoparticles in mice. We evaluated the protective capacity of CHKV-24 mAb immunoglobulin G protein or mRNA in mouse models of CHIKV infection. Treatment with CHKV-24 mRNA protected mice from arthritis, musculoskeletal tissue infection, and lethality and reduced viremia to undetectable levels at 2 days after inoculation. Infusion of macaques with CHKV-24 mRNA achieved a mean maximal mAb concentration of 10.1 to 35.9 micrograms per milliliter, with a half-life of 23 days, a level well above what is needed for protection in mice. Studies with CHKV-24 mRNA in macaques demonstrated a dose-response effect after the first dose of mRNA and maintained levels after second dose. These preclinical data with CHKV-24 mRNA suggest that it might be useful to prevent human disease.
Copyright © 2019 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.

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Year:  2019        PMID: 31101672      PMCID: PMC6629435          DOI: 10.1126/sciimmunol.aaw6647

Source DB:  PubMed          Journal:  Sci Immunol        ISSN: 2470-9468


  51 in total

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Journal:  Cancer Immunol Immunother       Date:  2017-08-17       Impact factor: 6.968

4.  Reovirus cell entry requires functional microtubules.

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5.  Efficient Targeting and Activation of Antigen-Presenting Cells In Vivo after Modified mRNA Vaccine Administration in Rhesus Macaques.

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Journal:  NPJ Vaccines       Date:  2017-07-06       Impact factor: 7.344

9.  A mouse model for Chikungunya: young age and inefficient type-I interferon signaling are risk factors for severe disease.

Authors:  Thérèse Couderc; Fabrice Chrétien; Clémentine Schilte; Olivier Disson; Madly Brigitte; Florence Guivel-Benhassine; Yasmina Touret; Georges Barau; Nadège Cayet; Isabelle Schuffenecker; Philippe Desprès; Fernando Arenzana-Seisdedos; Alain Michault; Matthew L Albert; Marc Lecuit
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Review 7.  Prophylactic strategies to control chikungunya virus infection.

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