Multivalent bicyclic peptides are an effective antiviral modality that can potently inhibit SARS-CoV-2

Author:

Gaynor Katherine U.ORCID,Vaysburd Marina,Harman Maximilian A. J.ORCID,Albecka Anna,Jeffrey Phillip,Beswick Paul,Papa GuidoORCID,Chen LiuhongORCID,Mallery DonnaORCID,McGuinness Brian,Van Rietschoten Katerine,Stanway Steven,Brear PaulORCID,Lulla Aleksei,Ciazynska KatarzynaORCID,Chang Veronica T.ORCID,Sharp JoORCID,Neary Megan,Box Helen,Herriott Jo,Kijak Edyta,Tatham Lee,Bentley Eleanor G.,Sharma Parul,Kirby Adam,Han Ximeng,Stewart James P.ORCID,Owen AndrewORCID,Briggs John A. G.ORCID,Hyvönen MarkoORCID,Skynner Michael J.ORCID,James Leo C.ORCID

Abstract

AbstractCOVID-19 has stimulated the rapid development of new antibody and small molecule therapeutics to inhibit SARS-CoV-2 infection. Here we describe a third antiviral modality that combines the drug-like advantages of both. Bicycles are entropically constrained peptides stabilized by a central chemical scaffold into a bi-cyclic structure. Rapid screening of diverse bacteriophage libraries against SARS-CoV-2 Spike yielded unique Bicycle binders across the entire protein. Exploiting Bicycles’ inherent chemical combinability, we converted early micromolar hits into nanomolar viral inhibitors through simple multimerization. We also show how combining Bicycles against different epitopes into a single biparatopic agent allows Spike from diverse variants of concern (VoC) to be targeted (Alpha, Beta, Delta and Omicron). Finally, we demonstrate in both male hACE2-transgenic mice and Syrian golden hamsters that both multimerized and biparatopic Bicycles reduce viraemia and prevent host inflammation. These results introduce Bicycles as a potential antiviral modality to tackle new and rapidly evolving viruses.

Funder

RCUK | Medical Research Council

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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