Novel analogues of a nonnucleoside SARS-CoV-2 RdRp inhibitor as potential antivirotics

Author:

Tóth Luca JuliannaORCID,Krejčová KateřinaORCID,Dejmek MilanORCID,Žilecká EvaORCID,Klepetářová Blanka,Poštová Slavětínská Lenka,Bouřa EvženORCID,Nencka RadimORCID

Abstract

The RNA-dependent RNA polymerase (RdRp) represents a prominent target in the discovery and development of new antivirotics against RNA viruses, inhibiting the replication process. One of the most targeted RNA viruses of the last years is, without doubt, SARS-CoV-2, the cause of the recent COVID-19 pandemic. HeE1-2Tyr, a known inhibitor of flaviviral RdRp, has been discovered to also have antiviral potency against this coronavirus. In this study, we report three distinct modifications of HeE1-2Tyr: conversion of the core from a benzothiazole to a benzoxazole moiety and two different scaffold simplifications, respectively. We provide a novel synthetic approach and, in addition, evaluate the final molecules in an in vitro polymerase assay for biological activity.

Funder

National Institute of virology and bacteriology

Ústav organické chemie a biochemie Akademie věd České republiky

Publisher

Beilstein Institut

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