AI Article Synopsis

  • Influenza viruses cause seasonal epidemics and occasional pandemics, necessitating the development of new antiviral drugs due to issues with existing treatments like oseltamivir, including drug resistance.
  • Researchers focused on creating AM2-S31N inhibitors as oral antivirals, finding promising candidates with strong antiviral properties and good pharmacokinetic (PK) profiles, particularly a compound identified as 10b.
  • Compound 10b shows enhanced antiviral effectiveness, works well in combination with oseltamivir, and demonstrates suitable characteristics for further testing in mouse models, indicating its potential as a new treatment option.

Article Abstract

Influenza viruses are respiratory pathogens that are responsible for both seasonal influenza epidemics and occasional influenza pandemics. The narrow therapeutic window of oseltamivir, coupled with the emergence of drug resistance, calls for the next-generation of antivirals. With our continuous interest in developing AM2-S31N inhibitors as oral influenza antivirals, we report here the progress of optimizing the in vitro pharmacokinetic (PK) properties of AM2-S31N inhibitors. Several AM2-S31N inhibitors, including compound 10b, were discovered to have potent channel blockage, single to submicromolar antiviral activity, and favorable in vitro PK properties. The antiviral efficacy of compound 10b was also synergistic with oseltamivir carboxylate. Interestingly, binding kinetic studies (K, K, and K) revealed several AM2-S31N inhibitors that have similar K values but significantly different K and K values. Overall, this study identified a potent lead compound (10b) with improved in vitro PK properties that is suitable for the in vivo mouse model studies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6445276PMC
http://dx.doi.org/10.1021/acs.jmedchem.7b01536DOI Listing

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