Literature DB >> 31175183

The L46P mutant confers a novel allosteric mechanism of resistance toward the influenza A virus M2 S31N proton channel blockers.

Rami Musharrafieh1, Panagiotis I Lagarias1, Chunlong Ma1, Gene S Tan1, Antonios Kolocouris2, Jun Wang3.   

Abstract

The Food and Drug Administration-approved influenza A antiviral amantadine inhibits the wild-type (WT) AM2 channel but not the S31N mutant predominantly found in circulating strains. In this study, serial viral passages were applied to select resistance against a newly developed isoxazole-conjugated adamantane inhibitor that targets the AM2 S31N channel. This led to the identification of the novel drug-resistant mutation L46P located outside the drug-binding site, which suggests an allosteric resistance mechanism. Intriguingly, when the L46P mutant was introduced to AM2 WT, the channel remained sensitive toward amantadine inhibition. To elucidate the molecular mechanism, molecular dynamics simulations and binding free energy molecular mechanics-generalized born surface area (MM-GBSA) calculations were performed on WT and mutant channels. It was found that the L46P mutation caused a conformational change in the N terminus of transmembrane residues 22-31 that ultimately broadened the drug-binding site of AM2 S31N inhibitor 4, which spans residues 26-34, but not of AM2 WT inhibitor amantadine, which spans residues 31-34. The MM-GBSA calculations showed stronger binding stability for 4 in complex with AM2 S31N compared with 4 in complex with AM2 S31N/L46P, and equal binding free energies of amantadine in complex with AM2 WT and AM2 L46P. Overall, these results demonstrate a unique allosteric resistance mechanism toward AM2 S31N channel blockers, and the L46P mutant represents the first experimentally confirmed drug-resistant AM2 mutant that is located outside of the pore where drug binds. SIGNIFICANCE STATEMENT: AM2 S31N is a high-profile antiviral drug target, as more than 95% of currently circulating influenza A viruses carry this mutation. Understanding the mechanism of drug resistance is critical in designing the next generation of AM2 S31N channel blockers. Using a previously developed AM2 S31N channel blocker as a chemical probe, this study was the first to identify a novel resistant mutant, L46P. The L46P mutant is located outside of the drug-binding site. Molecular dynamics simulations showed that L46P causes a dilation of drug-binding site between residues 22 and 31, which affects the binding of AM2 S31N channel blockers, but not the AM2 WT inhibitor amantadine.
Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.

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Year:  2019        PMID: 31175183      PMCID: PMC6608606          DOI: 10.1124/mol.119.116640

Source DB:  PubMed          Journal:  Mol Pharmacol        ISSN: 0026-895X            Impact factor:   4.436


  46 in total

1.  Distinct domains of the influenza a virus M2 protein cytoplasmic tail mediate binding to the M1 protein and facilitate infectious virus production.

Authors:  Matthew F McCown; Andrew Pekosz
Journal:  J Virol       Date:  2006-08       Impact factor: 5.103

2.  Discovery of novel dual inhibitors of the wild-type and the most prevalent drug-resistant mutant, S31N, of the M2 proton channel from influenza A virus.

Authors:  Jizhou Wang; Chunlong Ma; Jun Wang; Hyunil Jo; Belgin Canturk; Giacomo Fiorin; Lawrence H Pinto; Robert A Lamb; Michael L Klein; William F DeGrado
Journal:  J Med Chem       Date:  2013-03-27       Impact factor: 7.446

3.  A Robust Proton Flux (pHlux) Assay for Studying the Function and Inhibition of the Influenza A M2 Proton Channel.

Authors:  Paul Santner; João Miguel da Silva Martins; Jonas S Laursen; Lars Behrendt; Leise Riber; Christian A Olsen; Isaiah T Arkin; Jakob R Winther; Martin Willemoës; Kresten Lindorff-Larsen
Journal:  Biochemistry       Date:  2018-10-03       Impact factor: 3.162

4.  Free Energy Calculations by the Molecular Mechanics Poisson-Boltzmann Surface Area Method.

Authors:  Nadine Homeyer; Holger Gohlke
Journal:  Mol Inform       Date:  2012-01-10       Impact factor: 3.353

5.  Structure-Property Relationship Studies of Influenza A Virus AM2-S31N Proton Channel Blockers.

Authors:  Yanmei Hu; Raymond Kin Hau; Yuanxiang Wang; Peter Tuohy; Yongtao Zhang; Shuting Xu; Chunlong Ma; Jun Wang
Journal:  ACS Med Chem Lett       Date:  2018-10-03       Impact factor: 4.345

6.  The Influenza M2 Ectodomain Regulates the Conformational Equilibria of the Transmembrane Proton Channel: Insights from Solid-State Nuclear Magnetic Resonance.

Authors:  Byungsu Kwon; Mei Hong
Journal:  Biochemistry       Date:  2016-09-12       Impact factor: 3.162

7.  Functional studies indicate amantadine binds to the pore of the influenza A virus M2 proton-selective ion channel.

Authors:  Xianghong Jing; Chunlong Ma; Yuki Ohigashi; Fernando A Oliveira; Theodore S Jardetzky; Lawrence H Pinto; Robert A Lamb
Journal:  Proc Natl Acad Sci U S A       Date:  2008-07-31       Impact factor: 11.205

8.  Optimization of the additive CHARMM all-atom protein force field targeting improved sampling of the backbone φ, ψ and side-chain χ(1) and χ(2) dihedral angles.

Authors:  Robert B Best; Xiao Zhu; Jihyun Shim; Pedro E M Lopes; Jeetain Mittal; Michael Feig; Alexander D Mackerell
Journal:  J Chem Theory Comput       Date:  2012-07-18       Impact factor: 6.006

9.  Influenza virus A M2 protein generates negative Gaussian membrane curvature necessary for budding and scission.

Authors:  Nathan W Schmidt; Abhijit Mishra; Jun Wang; William F DeGrado; Gerard C L Wong
Journal:  J Am Chem Soc       Date:  2013-09-06       Impact factor: 15.419

10.  In Vitro Pharmacokinetic Optimizations of AM2-S31N Channel Blockers Led to the Discovery of Slow-Binding Inhibitors with Potent Antiviral Activity against Drug-Resistant Influenza A Viruses.

Authors:  Yuanxiang Wang; Yanmei Hu; Shuting Xu; Yongtao Zhang; Rami Musharrafieh; Raymond Kin Hau; Chunlong Ma; Jun Wang
Journal:  J Med Chem       Date:  2018-01-17       Impact factor: 7.446

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Journal:  Adv Exp Med Biol       Date:  2022       Impact factor: 2.622

2.  Investigation of the Drug Resistance Mechanism of M2-S31N Channel Blockers through Biomolecular Simulations and Viral Passage Experiments.

Authors:  Rami Musharrafieh; Panagiotis Lagarias; Chunlong Ma; Raymond Hau; Alex Romano; George Lambrinidis; Antonios Kolocouris; Jun Wang
Journal:  ACS Pharmacol Transl Sci       Date:  2020-03-31

3.  Site-directed M2 proton channel inhibitors enable synergistic combination therapy for rimantadine-resistant pandemic influenza.

Authors:  Claire Scott; Jayakanth Kankanala; Toshana L Foster; Daniel H Goldhill; Peng Bao; Katie Simmons; Marieke Pingen; Matthew Bentham; Elizabeth Atkins; Eleni Loundras; Ruth Elderfield; Jolyon K Claridge; Joseph Thompson; Peter R Stilwell; Ranjitha Tathineni; Clive S McKimmie; Paul Targett-Adams; Jason R Schnell; Graham P Cook; Stephen Evans; Wendy S Barclay; Richard Foster; Stephen Griffin
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Authors:  Elnaz Aledavood; Beatrice Selmi; Carolina Estarellas; Matteo Masetti; F Javier Luque
Journal:  Front Mol Biosci       Date:  2022-01-14

Review 5.  Put a cork in it: Plugging the M2 viral ion channel to sink influenza.

Authors:  Pouria H Jalily; Maggie C Duncan; David Fedida; Jun Wang; Ian Tietjen
Journal:  Antiviral Res       Date:  2020-03-27       Impact factor: 5.970

6.  Rational design of a deuterium-containing M2-S31N channel blocker UAWJ280 with in vivo antiviral efficacy against both oseltamivir sensitive and -resistant influenza A viruses.

Authors:  C Joaquín Cáceres; Yanmei Hu; Stivalis Cárdenas-García; Xiangmeng Wu; Haozhou Tan; Silvia Carnaccini; L Claire Gay; Ginger Geiger; Chunlong Ma; Qing-Yu Zhang; Daniela Rajao; Daniel R Perez; Jun Wang
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7.  Clinically Relevant Influenza Virus Evolution Reconstituted in a Human Lung Airway-on-a-Chip.

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  7 in total

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