RXP 407, a phosphinic peptide, is a potent inhibitor of angiotensin I converting enzyme able to differentiate between its two active sites
10.1073/pnas.96.8.4330
Crossref journal-article
Proceedings of the National Academy of Sciences
Proceedings of the National Academy of Sciences (341)
Abstract

The human somatic angiotensin converting enzyme (ACE) contains two homologous domains, each bearing a zinc-dependent active site. All of the synthetic inhibitors of this enzyme used in clinical applications interact with these two active sites to a similar extent. Recently, several lines of evidence have suggested that the N-terminal active site of ACE might be involved in specific hydrolysis of some important physiological substrates, like Acetyl-Seryl-Aspartyl-Lysyl-Proline, a negative regulator of hematopoietic stem cell differentiation and proliferation. These findings have stimulated studies aimed at identifying new ACE inhibitors able to block only one of the two active sites of this enzyme. By screening phosphinic peptide libraries, we discovered a phosphinic peptide Ac-Asp-(L)Pheψ(PO2-CH2)(L)Ala-Ala-NH2, called RXP 407, which is able to differentiate the two ACE active sites, with a dissociation constant three orders of magnitude lower for the N-domain of the enzyme. The usefulness of a combinatorial chemistry approach to develop new lead structures is underscored by the unusual chemical structure of RXP 407, as compared with classical ACE inhibitors. As a highly potent and selective inhibitor of the N-terminal active site of wild ACE (Ki= 12 nM), RXP 407, which is metabolically stablein vivo, may lead to a new generation of ACE inhibitors able to blockin vivoonly a subset of the different functions regulated by ACE.

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Dive, V., Cotton, J., Yiotakis, A., Michaud, A., Vassiliou, S., Jiracek, J., Vazeux, G., Chauvet, M.-T., Cuniasse, P., & Corvol, P. (1999). RXP 407, a phosphinic peptide, is a potent inhibitor of angiotensin I converting enzyme able to differentiate between its two active sites. Proceedings of the National Academy of Sciences, 96(8), 4330–4335.

Authors 10
  1. Vincent Dive (first)
  2. Joël Cotton (additional)
  3. Athanasios Yiotakis (additional)
  4. Annie Michaud (additional)
  5. Stamatia Vassiliou (additional)
  6. Jiri Jiracek (additional)
  7. Gilles Vazeux (additional)
  8. Marie-Thérèse Chauvet (additional)
  9. Philippe Cuniasse (additional)
  10. Pierre Corvol (additional)
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Dates
Type When
Created 23 years, 1 month ago (July 26, 2002, 10:42 a.m.)
Deposited 1 year, 8 months ago (Jan. 4, 2024, 12:06 a.m.)
Indexed 2 weeks, 3 days ago (Aug. 19, 2025, 5:56 a.m.)
Issued 26 years, 4 months ago (April 13, 1999)
Published 26 years, 4 months ago (April 13, 1999)
Published Online 26 years, 4 months ago (April 13, 1999)
Published Print 26 years, 4 months ago (April 13, 1999)
Funders 0

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@article{Dive_1999, title={RXP 407, a phosphinic peptide, is a potent inhibitor of angiotensin I converting enzyme able to differentiate between its two active sites}, volume={96}, ISSN={1091-6490}, url={http://dx.doi.org/10.1073/pnas.96.8.4330}, DOI={10.1073/pnas.96.8.4330}, number={8}, journal={Proceedings of the National Academy of Sciences}, publisher={Proceedings of the National Academy of Sciences}, author={Dive, Vincent and Cotton, Joël and Yiotakis, Athanasios and Michaud, Annie and Vassiliou, Stamatia and Jiracek, Jiri and Vazeux, Gilles and Chauvet, Marie-Thérèse and Cuniasse, Philippe and Corvol, Pierre}, year={1999}, month=apr, pages={4330–4335} }