Arabian Journal of Chemistry (Feb 2023)

Diastereoselective synthesis of a novel phosphinic peptide as ACE inhibitor: Fragment-based design approach

  • Moaz M. Abdou,
  • Dewen Dong,
  • Paul M. O'Neill,
  • Eric Amigues,
  • Magdalini Matziari

Journal volume & issue
Vol. 16, no. 2
p. 104499

Abstract

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In medicinal chemistry for the purpose of lead optimization, hit selection of new isofunctional chemotypes are crucial for the success of identifying novel chemical entities of increased potency. Using fragment-based design approach with the N-selective inhibitor RXP407, a novel phosphinic peptide scaffold that consisted of modified RXP407 fragments was generated. The presented synthetic route is straightforward and produces the desired product Z-RXP407 in moderate yield. The (S,R,S,S)-Z-RXP407 analog has been evaluated for the C- and N-domain constructs of angiotensin-converting enzyme. The potency of this analog has been much lower compared to the parent compound RXP407, providing thus valuable insights regarding further design based on structure–activity relationships.

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