Novel renin inhibitors containing derivatives of N-alkylleucyl-β-hydroxy-γ-amino acids

Iwona Winiecka; Paweł Jaworski; Aleksander Paweł Mazurek; Dorota Marszałek; Anna Goldnik; Daniel Sokulski

doi:10.1002/psc.2846

Novel renin inhibitors containing derivatives of N-alkylleucyl-β-hydroxy-γ-amino acids

J Pept Sci. 2016 Feb;22(2):106-15. doi: 10.1002/psc.2846. Epub 2016 Jan 19.

Authors

Iwona Winiecka¹, Paweł Jaworski¹, Aleksander Paweł Mazurek¹, Dorota Marszałek¹, Anna Goldnik¹, Daniel Sokulski¹

Affiliation

¹ Department of Drug Chemistry, Medical University of Warsaw, Banacha 1, 02 - 097, Warsaw, Poland.

PMID: 26780837
DOI: 10.1002/psc.2846

Abstract

In search for new drugs lowering arterial blood pressure, which could be applied in anti-hypertensive therapy, research concerning agents blocking of renin-angiotensin-aldosteron system has been conducted. Despite many years of research conducted at many research centers around the world, aliskiren is the only one renin inhibitor, which is used up to now. Four novel potential renin inhibitors, having structure based on the peptide fragment 8-13 of human angiotensinogen, a natural substrate for renin, were designed and synthesized. All these inhibitors contain unnatural moieties that are derivatives of N-methylleucyl-β-hydroxy-γ-amino acids at the P2-P1' position: 4-[N-(N-methylleucyl)-amino]-3-hydroxy-7-(3-nitroguanidino)-heptanoic acid (AHGHA), 4-[N-(N-methylleucyl)-amino]-3-hydroxy-5-phenyl-pentanoic acid (AHPPA) or 4-[N-(N-methylleucyl)-amino]-8-benzyloxycarbonylamino-3-hydroxyoctanoic acid (AAHOA). The previously listed synthetic β-hydroxy-γ-amino acids constitute pseudodipeptidic units that correspond to the P1-P1' position of the inhibitor molecule. An unnatural amino acid, 4-methoxyphenylalanin (Phe(4-OMe)), was introduced at the P3 position of the obtained compounds. Three of these compounds contain isoamylamide of 6-aminohexanoic acid (ε-Ahx-Iaa) at the P2'-P3' position. The proposed modifications of the selected human angiotensinogen fragment are intended to increase bioactivity, bioavailability, and stability of the inhibitor molecule in body fluids and tissues. The inhibitor Boc-Phe(4-OMe)-MeLeu-AHGHA-OEt was obtained in the form of an ethyl ester. The hydrophobicity coefficient, expressed as log P varied between 3.95 and 8.17. In vitro renin inhibitory activity of all obtained compounds was contained within the range 10(-6)-10(-9) M. The compound Boc-Phe(4-OMe)-MeLeu-AHPPA-Ahx-Iaa proved to be the most active (IC50 = 1.05 × 10(-9) M). The compounds Boc-Phe(4-OMe)-MeLeu-AHGHA-Ahx-Iaa and Boc-Phe(4-OMe)-MeLeu-AHPPA-Ahx-Iaa are resistant to chymotrypsin.

Keywords: amino acids; hypertension treatment; pseudodipeptidic unit; renin inhibitors.

MeSH terms

Angiotensins / chemistry
Fatty Acids / chemistry*
Humans
Leucine / analogs & derivatives*
Leucine / chemistry*
Models, Molecular
Protease Inhibitors / chemistry*
Renin / antagonists & inhibitors*
Renin / chemistry

Substances

Angiotensins
Fatty Acids
Protease Inhibitors
Renin
Leucine