Effect of N-[(S)-1-carboxy-3-phenylpropyl]-L-Ala-L-Pro and Its Ethyl Ester (MK-421) on Angiotensin Converting Enzyme in Vitro and Angiotensin I Pressor Responses in Vivo

Overview

Journal J Pharmacol Exp Ther

Specialty Pharmacology

Date 1981 Mar 1

PMID 6259322

Citations 30

Authors

D M Gross

C S Sweet

E H Ulm

E P Backlund

A A MORRIS

D Weitz

D L Bohn

H C WENGER

T C Vassil

C A Stone

Affiliations

Soon will be listed here.

Abstract

The parent diacid (N-[(S)-1-carboxy-3-phenylpropyl]-L-Ala-L-Pro of MK-421 inhibited hog plasma angiotensin converting enzyme (ACE) by 50% (I50) at a concentration of 1.2 nM and was 17 times more potent than captopril. In vitro the I50 for MK-421, an ethyl ester, was 1200 nM because de-esterification did not occur. Similarly in the guinea-pig ileum, the diacid inhibitor and MK-421 potentiated the contractile effects of bradykinin at an AC50 of 77 pM and 18 nM, respectively. Inhibition of the pressor effects of angiotensin I by the diacid ACE inhibitor occurred at an ID50 of 8.2 micrograms/kg i.v. in rats and 6.4 micrograms/kg i.v. in dogs. Thus, the diacid was approximately 12 times more potent than captopril. The ID50 for MK-421 was 14 and 278 micrograms/kg i.v. in rats and dogs, respectively, because of differences in the rates of de-esterification. Oral ACE inhibitory activity was determined by blockade of the pressor effects of angiotensin I in conscious rats and dogs. In rats, but not in dogs, the diacid inhibitor was poorly absorbed, whereas MK-421 was well absorbed in both species. MK-421 inhibited the pressor effects of angiotensin I at 0.1 to 3.0 mg/kg p.o. for at least 6 hr in rats and dogs, and compared to captopril was 8.6 times more potent in rats and 4.6 times more potent in dogs. These data demonstrate that MK-421 and its parent diacid are potent, long-lasting orally active inhibitors of ACE. In addition, the low activity of MK-421 in vitro contrasts with its substantial in vivo activity, and supports the hypothesis that MK-421 is a prodrug that first must be de-esterified to permit full expression of its significant in vivo pharmacological activity.

Citing Articles

Diallyl sulfide protects against dilated cardiomyopathy via inhibition of oxidative stress and apoptosis in mice.

Pang S, Dong W, Liu N, Gao S, Li J, Zhang X Mol Med Rep. 2021; 24(6).

PMID: 34651661 PMC: 8532119. DOI: 10.3892/mmr.2021.12492.

A Phosphoramidate Strategy Enables Membrane Permeability of a Non-nucleotide Inhibitor of the Prolyl Isomerase Pin1.

Schwarz D, Williams S, Dillenburg M, Wagner C, Gestwicki J ACS Med Chem Lett. 2020; 11(9):1704-1710.

PMID: 32944137 PMC: 7488286. DOI: 10.1021/acsmedchemlett.0c00170.

Knowledge-based structural models of SARS-CoV-2 proteins and their complexes with potential drugs.

Hijikata A, Shionyu-Mitsuyama C, Nakae S, Shionyu M, Ota M, Kanaya S FEBS Lett. 2020; 594(12):1960-1973.

PMID: 32379896 PMC: 7267562. DOI: 10.1002/1873-3468.13806.

Secoisolariciresinol Diglucoside (SDG) Isolated from Flaxseed, an Alternative to ACE Inhibitors in the Treatment of Hypertension.

Prasad K Int J Angiol. 2014; 22(4):235-8.

PMID: 24436618 PMC: 3830572. DOI: 10.1055/s-0033-1351687.

Roles of proteolysis in regulation of GPCR function.

Cottrell G Br J Pharmacol. 2012; 168(3):576-90.

PMID: 23043558 PMC: 3579280. DOI: 10.1111/j.1476-5381.2012.02234.x.