The substitutions L50F, E166A and L167F in SARS-CoV-2 3CLpro are selected by a protease inhibitor in vitro and confer resistance to nirmatrelvir

Dirk Jochmans; Cheng Liu; Kim Donckers; Antitsa Stoycheva; Sandro Boland; Sarah K Stevens; Chloe De Vita; Bert Vanmechelen; Piet Maes; Bettina Salome Trüeb; Nadine Ebert; Volker Thiel; Steven De Jonghe; Laura Vangeel; Dorothée Bardiot; Andreas Jekle; Lawrence M Blatt; Leonid Beigelman; Julian A Symons; Pierre Raboisson; Patrick Chaltin; Arnaud Marchand; Johan Neyts; Jerome Deval; Koen Vandyck

Este artigo é um Preprint

Preprints são relatos preliminares de pesquisa que não foram certificados pela revisão por pares. Eles não devem ser considerados para orientar a prática clínica ou comportamentos relacionados à saúde e não devem ser publicados na mídia como informação estabelecida.

Preprints publicados online permitem que os autores recebam feedback rápido, e toda a comunidade científica pode avaliar o trabalho independentemente e responder adequadamente. Estes comentários são publicados juntamente com os preprints para qualquer pessoa ler e servir como uma avaliação pós-publicação.

The substitutions L50F, E166A and L167F in SARS-CoV-2 3CLpro are selected by a protease inhibitor in vitro and confer resistance to nirmatrelvir

Dirk Jochmans; Cheng Liu; Kim Donckers; Antitsa Stoycheva; Sandro Boland; Sarah K Stevens; Chloe De Vita; Bert Vanmechelen; Piet Maes; Bettina Salome Trüeb; Nadine Ebert; Volker Thiel; Steven De Jonghe; Laura Vangeel; Dorothée Bardiot; Andreas Jekle; Lawrence M Blatt; Leonid Beigelman; Julian A Symons; Pierre Raboisson; Patrick Chaltin; Arnaud Marchand; Johan Neyts; Jerome Deval; Koen Vandyck.

Afiliação

Dirk Jochmans; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Virology & Chemotherapy, Herestraat 49, 3000 Leuven, Belgium
Cheng Liu; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Kim Donckers; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Virology & Chemotherapy, Herestraat 49, 3000 Leuven, Belgium
Antitsa Stoycheva; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Sandro Boland; CISTIM Leuven vzw, Gaston Geenslaan 2, 3001 Leuven, Belgium
Sarah K Stevens; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Chloe De Vita; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Bert Vanmechelen; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Clinical & Epidemiological Virology, Herestraat 49, Leuven, 3
Piet Maes; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Clinical & Epidemiological Virology, Herestraat 49, Leuven, 3
Bettina Salome Trüeb; Institute of Virology and Immunology, University of Bern, 3012, Bern, Switzerland; Department of Infectious Diseases and Pathobiology, Vetsuisse Faculty, Univer
Nadine Ebert; Institute of Virology and Immunology, University of Bern, 3012, Bern, Switzerland; Department of Infectious Diseases and Pathobiology, Vetsuisse Faculty, Univer
Volker Thiel; Institute of Virology and Immunology, University of Bern, 3012, Bern, Switzerland; Department of Infectious Diseases and Pathobiology, Vetsuisse Faculty, Univer
Steven De Jonghe; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Virology & Chemotherapy, Herestraat 49, 3000 Leuven, Belgium
Laura Vangeel; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Virology & Chemotherapy, Herestraat 49, 3000 Leuven, Belgium
Dorothée Bardiot; CISTIM Leuven vzw, Gaston Geenslaan 2, 3001 Leuven, Belgium
Andreas Jekle; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Lawrence M Blatt; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Leonid Beigelman; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Julian A Symons; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Pierre Raboisson; Aligos Belgium BV, Gaston Geenslaan 1, 3001 Leuven, Belgium
Patrick Chaltin; Centre for Drug Design and Discovery (CD3), KU Leuven, Gaston Geenslaan 2, 3001 Leuven, Belgium; CISTIM Leuven vzw, Gaston Geenslaan 2, 3001 Leuven, Belgium
Arnaud Marchand; CISTIM Leuven vzw, Gaston Geenslaan 2, 3001 Leuven, Belgium
Johan Neyts; KU Leuven, Department of Microbiology, Immunology & Transplantation, Rega Institute, Laboratory of Virology & Chemotherapy, Herestraat 49, 3000 Leuven, Belgium
Jerome Deval; Aligos Therapeutics, Inc., 1 Corporate Dr., 2nd Floor, South San Francisco, CA, USA
Koen Vandyck; Aligos Belgium BV, Gaston Geenslaan 1, 3001 Leuven, Belgium

Preprint em Inglês | bioRxiv | ID: ppbiorxiv-495116

ABSTRACT

ABSTRACT

The SARS-CoV-2 main protease (3CLpro) has an indispensable role in the viral life cycle and is a therapeutic target for the treatment of COVID-19. The potential of 3CLpro-inhibitors to select for drug-resistant variants needs to be established. Therefore, SARS-CoV-2 was passaged in vitro in the presence of increasing concentrations of ALG-097161, a probe compound designed in the context of a 3CLpro drug discovery program. We identified a combination of amino acid substitutions in 3CLpro (L50F E166A L167F) that is associated with > 20x increase in EC50 values for ALG-097161, nirmatrelvir (PF-07321332) and PF-00835231. While two of the single substitutions (E166A and L167F) provide low-level resistance to the inhibitors in a biochemical assay, the triple mutant results in the highest levels of resistance (6x to 72x). All substitutions are associated with a significant loss of enzymatic 3CLpro activity, suggesting a reduction in viral fitness. Structural biology analysis indicates that the different substitutions reduce the number of inhibitor/enzyme interactions while the binding of the substrate is maintained. These observations will be important for the interpretation of resistance development to 3CLpro inhibitors in the clinical setting. Abstract ImportancePaxlovid is the first oral antiviral approved for treatment of SARS-CoV-2 infection. Antiviral treatments are often associated with the development of drug resistant viruses. In order to guide the use of novel antivirals it is essential to understand the risk of resistance development and to characterize the associated changes in the viral genes and proteins. In this work, we describe for the first time a pathway that allows SARS-CoV-2 to develop resistance against Paxlovid in vitro. The characteristics of in vitro antiviral resistance development may be predictive for the clinical situation. Therefore, our work will be important for the management of COVID-19 with Paxlovid and next generation SARS-CoV-2 3CLpro inhibitors.

Licença

cc_by_nc_nd

Texto completo

Adicionar na Minha BVS

Imprimir

XML

Buscar no Google

Texto completo: Disponível Coleções: Preprints Base de dados: bioRxiv Tipo de estudo: Estudo observacional / Estudo prognóstico Idioma: Inglês Ano de publicação: 2022 Tipo de documento: Preprint

Texto completo

Adicionar na Minha BVS

Imprimir

XML

Buscar no Google