Literature DB >> 28087313

An M2-V27A channel blocker demonstrates potent in vitro and in vivo antiviral activities against amantadine-sensitive and -resistant influenza A viruses.

Yanmei Hu1, Rami Musharrafieh2, Chunlong Ma3, Jiantao Zhang1, Donald F Smee4, William F DeGrado5, Jun Wang1,3.   

Abstract

Adamantanes such as amantadine (1) and rimantadine (2) are FDA-approved anti-influenza drugs that act by inhibiting the wild-type M2 proton channel from influenza A viruses, thereby inhibiting the uncoating of the virus. Although adamantanes have been successfully used for more than four decades, their efficacy was curtailed by emerging drug resistance. Among the limited number of M2 mutants that confer amantadine resistance, the M2-V27A mutant was found to be the predominant mutant under drug selection pressure, thereby representing a high profile antiviral drug target. Guided by molecular dynamics simulations, we previously designed first-in-class M2-V27A inhibitors. One of the potent lead compounds, spiroadamantane amine (3), inhibits both the M2-WT and M2-V27A mutant with IC50 values of 18.7 and 0.3 μM, respectively, in in vitro electrophysiological assays. Encouraged by these findings, in this study we further examine the in vitro and in vivo antiviral activity of compound 3 in inhibiting both amantadine-sensitive and -resistant influenza A viruses. Compound 3 not only had single to sub-micromolar EC50 values against M2-WT- and M2-V27A-containing influenza A viruses in antiviral assays, but also rescued mice from lethal viral infection by either M2-WT- or M2-V27A-containing influenza A viruses. In addition, we report the design of two analogs of compound 3, and one was found to have improved in vitro antiviral activity over compound 3. Collectively, this study represents the first report demonstrating the in vivo antiviral efficacy of inhibitors targeting M2 mutants. The results suggest that inhibitors targeting drug-resistant M2 mutants are promising antiviral drug candidates worthy of further development.
Copyright © 2017 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Antiviral; Drug resistance; Influenza virus; M2 proton channel; Spiroadamantane; V27A

Mesh:

Substances:

Year:  2017        PMID: 28087313      PMCID: PMC5326599          DOI: 10.1016/j.antiviral.2017.01.006

Source DB:  PubMed          Journal:  Antiviral Res        ISSN: 0166-3542            Impact factor:   5.970


  36 in total

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Authors:  Matthew G Durrant; Dennis L Eggett; David D Busath
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2.  Profiling the in vitro drug-resistance mechanism of influenza A viruses towards the AM2-S31N proton channel blockers.

Authors:  Rami Musharrafieh; Chunlong Ma; Jun Wang
Journal:  Antiviral Res       Date:  2018-03-06       Impact factor: 5.970

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

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Journal:  ACS Med Chem Lett       Date:  2018-10-03       Impact factor: 4.345

5.  Slow but Steady Wins the Race: Dissimilarities among New Dual Inhibitors of the Wild-Type and the V27A Mutant M2 Channels of Influenza A Virus.

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7.  Increased Dissociation of Adamantanamines in Influenza A M2 S31N with Partial Block by Rimantadine.

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8.  Inhibitors of the M2 Proton Channel Engage and Disrupt Transmembrane Networks of Hydrogen-Bonded Waters.

Authors:  Jessica L Thomaston; Nicholas F Polizzi; Athina Konstantinidi; Jun Wang; Antonios Kolocouris; William F DeGrado
Journal:  J Am Chem Soc       Date:  2018-09-12       Impact factor: 15.419

9.  X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance.

Authors:  Jessica L Thomaston; Athina Konstantinidi; Lijun Liu; George Lambrinidis; Jingquan Tan; Martin Caffrey; Jun Wang; William F Degrado; Antonios Kolocouris
Journal:  Biochemistry       Date:  2020-01-13       Impact factor: 3.162

10.  Discovery of M2 channel blockers targeting the drug-resistant double mutants M2-S31N/L26I and M2-S31N/V27A from the influenza A viruses.

Authors:  Rami Musharrafieh; Chunlong Ma; Jun Wang
Journal:  Eur J Pharm Sci       Date:  2019-11-05       Impact factor: 4.384

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