An oral SARS-CoV-2 M <sup>pro</sup> inhibitor clinical candidate for the treatment of COVID-19

Dafydd R. Owen , Charlotte Allerton , Annaliesa S. Anderson , Dafydd R. Owen , Charlotte Allerton , Annaliesa S. Anderson , Lisa Aschenbrenner , Melissa Avery , Simon Berritt , Britton Boras , Rhonda D. Cardin , Anthony Carlo , Karen J. Coffman , Alyssa Dantonio , Li Di , Heather Eng , Rose Ann Ferre , K.S. Gajiwala , Scott Gibson , S.E. Greasley , Brett L. Hurst , Eugene P. Kadar , Amit S. Kalgutkar , Jack C. Lee , Jisun Lee , Wei Liu , Stephen W. Mason , Stephen Noell , Jonathan J. Novak , R. Scott Obach , Kevin Ogilvie , Nandini C. Patel , Martin Pettersson , K. Devendra , Matthew R. Reese , M. F. Sammons , Jean G. Sathish , Ravi Shankar Prasad Singh , Claire M. Steppan , Al Stewart , Jamison B. Tuttle , Lawrence W. Updyke , Patrick R. Verhoest , Liuqing Wei , Qingyi Yang , Yuao Zhu
2021 Science 1,754 citations

Abstract

Path to another drug against COVID-19 The rapid development of vaccines has been crucial in battling the ongoing COVID-19 pandemic. However, access challenges remain, breakthrough infections occur, and emerging variants present increased risk. Developing antiviral therapeutics is therefore a high priority for the treatment of COVID-19. Some drug candidates in clinical trials act against the viral RNA-dependent RNA polymerase, but there are other viral enzymes that have been considered good targets for inhibition by drugs. Owen et al . report the discovery and characterization of a drug against the main protease involved in the cleavage of polyproteins involved in viral replication. The drug, PF-07321332, can be administered orally, has good selectivity and safety profiles, and protects against infection in a mouse model. In a phase 1 clinical trial, the drug reached concentrations expected to inhibit the virus based on in vitro studies. It also inhibited other coronaviruses, including severe acute respiratory syndrome coronavirus 1 and Middle East respiratory syndrome coronavirus, and could be in the armory against future viral threats. —VV

Keywords

PotencyOutbreakCoronavirus disease 2019 (COVID-19)In vivoVirologyPandemicCoronavirusSevere acute respiratory syndrome coronavirus 2 (SARS-CoV-2)Clinical trialPharmacologyIn vitroProtease inhibitor (pharmacology)MedicineChemistryBiologyVirusViral loadDiseaseInternal medicineBiochemistryInfectious disease (medical specialty)Biotechnology

MeSH Terms

AdministrationOralAnimalsCOVID-19Clinical TrialsPhase I as TopicCoronavirusDisease ModelsAnimalDrug TherapyCombinationHumansLactamsLeucineMiceMiceInbred BALB CMicrobial Sensitivity TestsNitrilesProlineRandomized Controlled Trials as TopicRitonavirSARS-CoV-2Viral Protease InhibitorsVirus ReplicationCOVID-19 Drug Treatment

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Publication Info

Year
2021
Type
article
Volume
374
Issue
6575
Pages
1586-1593
Citations
1754
Access
Closed

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Dafydd R. Owen, Charlotte Allerton, Annaliesa S. Anderson et al. (2021). An oral SARS-CoV-2 M <sup>pro</sup> inhibitor clinical candidate for the treatment of COVID-19. Science , 374 (6575) , 1586-1593. https://doi.org/10.1126/science.abl4784

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DOI
10.1126/science.abl4784
PMID
34726479

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Data completeness: 86%