AI Article Synopsis

  • Researchers developed new classes of donepezil analogues and prodrugs to improve inhibition of hAChE and eqBuChE, synthesizing over 70 compounds.
  • Most of the prodrugs showed low activity against AChE, while the N-benzylpyridinium salts displayed strong inhibitory effects, with some achieving subnanomolar activity.
  • The study also examined stereogenic centers' impact on activity and oxidation rates, providing valuable insights for advancing the "bio-oxidizable" prodrug strategy in preclinical development.

Article Abstract

As an extension of our previous work on donepezil-based "bio-oxidizable" prodrug approach, two new classes of N-benzylpyridinium donepezil analogues in tetralone B2 and acetophenone B3 series and a new set of indanone derivatives B1 were investigated along with the corresponding dihydropyridine prodrugs A1-3. A total of fifty one N-benzylpyridinium quaternary donepezil analogues B1-3 and twenty two prodrugs A1-3 were synthesized and evaluated for their inhibitory activities against hAChE and eqBuChE. While most prodrugs A1-3 were demonstrated to be inactive against AChE (IC > 10 μM), a large number of the corresponding N-benzylpyridinium salt B1-3 exhibited appealing three-to-one-digit nanomolar hAChE inhibitory activities and even reaching subnanomolar activity (IC = 0.36 nM). In addition, in silico docking studies were conducted for several compounds to explain the more relevant in vitro results. Lastly, the influence of the two stereogenic centers in prodrugs A was also evaluated, highlighting not only marked differences in residual AChE inhibitory activity of the four separated isomers of prodrug 23h (IC ranging from 173 nM to 10 μM) but also significant variations of the oxidation rate between two separated diastereoisomers of prodrug 24a. This work provides useful information in the search of a preclinical candidate to conduct further development of this attractive "bio-oxidizable" prodrug strategy.

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Source
http://dx.doi.org/10.1016/j.ejmech.2017.12.084DOI Listing

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