A therapeutic combination of two small molecule toxin inhibitors provides broad preclinical efficacy against viper snakebite

Author:

Albulescu Laura-Oana,Xie Chunfang,Ainsworth Stuart,Alsolaiss Jaffer,Crittenden Edouard,Dawson Charlotte A.ORCID,Softley Rowan,Bartlett Keirah E.,Harrison Robert A.,Kool JeroenORCID,Casewell Nicholas R.ORCID

Abstract

AbstractSnakebite is a medical emergency causing high mortality and morbidity in rural tropical communities that typically experience delayed access to unaffordable therapeutics. Viperid snakes are responsible for the majority of envenomings, but extensive interspecific variation in venom composition dictates that different antivenom treatments are used in different parts of the world, resulting in clinical and financial snakebite management challenges. Here, we show that a number of repurposed Phase 2-approved small molecules are capable of broadly neutralizing distinct viper venom bioactivities in vitro by inhibiting different enzymatic toxin families. Furthermore, using murine in vivo models of envenoming, we demonstrate that a single dose of a rationally-selected dual inhibitor combination consisting of marimastat and varespladib prevents murine lethality caused by venom from the most medically-important vipers of Africa, South Asia and Central America. Our findings support the translation of combinations of repurposed small molecule-based toxin inhibitors as broad-spectrum therapeutics for snakebite.

Funder

Wellcome Trust

RCUK | Medical Research Council

Royal Society

Publisher

Springer Science and Business Media LLC

Subject

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

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