Novel activity of endothelin-converting enzyme: hydrolysis of bradykinin

被引：90

作者：

Hoang, MV ^{[1
]}

Turner, AJ ^{[1
]}

机构：

[1] UNIV LEEDS,SCH BIOCHEM & MOL BIOL,LEEDS LS2 9JT,W YORKSHIRE,ENGLAND

来源：

BIOCHEMICAL JOURNAL | 1997年 / 327卷

关键词：

D O I：

10.1042/bj3270023

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Endothelin-converting enzyme (ECE) is the key enzyme in the production of the potent vasoconstrictor endothelin from its inactive precursor big endothelin. To date, no other physiological peptide substrate has been identified for ECE. Here, by using Chinese hamster ovary (CHO) cells transfected with rat ECE-1 cDNA, we have established that ECE can hydrolyse the vasodilator bradykinin. The hydrolysis of bradykinin by ECE is exclusively at the Pro(7)-Phe(8) bond, producing bradykinin-(1-7) and bradykinin-(8-9), Hydrolysis is completely inhibited by 100 mu M phosphoramidon and 200 mu M EDTA, but only slightly by the specific neprilysin inhibitor thiorphan (100 mu M). The ability of ECE to act as a peptidyl dipeptidase rather than an endopeptidase in hydrolysing bradykinin suggests a much broader specificity for the enzyme than previously recognized, which may lead to the design of new and specific inhibitors of ECE and to the identification of other potential physiological substrates.

引用

页码：23 / 26

页数：4

共 23 条

[1]

BARNES K, 1997, IN PRESS HYPERTENSIO

[2]

BARNES L, 1995, J CARDIOVASC PHAR S3, V26, pS37

[3] The conformation of human big endothelin-1 favours endopeptidase hydrolysis of the TRP(21)-VAL(22) bond [J].

Corder, R .

BIOCHEMICAL PHARMACOLOGY, 1996, 51 (03) :259-266

[4] ENZYMATIC INACTIVATION OF BRADYKININ BY RAT-BRAIN NEURONAL PERIKARYA [J].

DELBEL, EA ;

PADOVAN, AP ;

PADOVAN, GJ ;

SELLINGER, OZ ;

MARTINS, AR .

CELLULAR AND MOLECULAR NEUROBIOLOGY, 1989, 9 (03) :379-400

[5] PROCESSING OF PROENDOTHELIN-1 BY HUMAN FURIN CONVERTASE [J].

DENAULT, JB ;

CLAING, A ;

DORLEANSJUSTE, P ;

SAWAMURA, T ;

KIDO, T ;

MASAKI, T ;

LEDUC, R .

FEBS LETTERS, 1995, 362 (03) :276-280

[6] INVIVO EXPRESSION OF MUTANT PREPROENDOTHELINS - HIERARCHY OF PROCESSING EVENTS BUT NO STRICT REQUIREMENT OF TRP-VAL AT THE PROCESSING SITE [J].

FABBRINI, MS ;

VITALE, A ;

PEDRAZZINI, E ;

NITTI, G ;

ZAMAI, M ;

TAMBURIN, M ;

CAIOLFA, VR ;

PATRONO, C ;

BENATTI, L .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (09) :3923-3927

[7] Mutagenesis and modelling of endothelin converting enzyme [J].

Hoang, VM ;

Sansom, CE ;

Turner, AJ .

BIOCHEMICAL SOCIETY TRANSACTIONS, 1996, 24 (03) :S471-S471

[8] THE HUMAN ENDOTHELIN FAMILY - 3 STRUCTURALLY AND PHARMACOLOGICALLY DISTINCT ISOPEPTIDES PREDICTED BY 3 SEPARATE GENES [J].

INOUE, A ;

YANAGISAWA, M ;

KIMURA, S ;

KASUYA, Y ;

MIYAUCHI, T ;

GOTO, K ;

MASAKI, T .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (08) :2863-2867

[9] CLEAVAGE OF STRUCTURAL PROTEINS DURING ASSEMBLY OF HEAD OF BACTERIOPHAGE-T4 [J].

LAEMMLI, UK .

NATURE, 1970, 227 (5259) :680-+

[10] Endothelin-converting enzyme expression in the rat vascular injury model and human coronary atherosclerosis [J].

Minamino, T ;

Kurihara, H ;

Takahashi, M ;

Shimada, K ;

Maemura, K ;

Oda, H ;

Ishikawa, T ;

Uchiyama, T ;

Tanzawa, K ;

Yazaki, Y .

CIRCULATION, 1997, 95 (01) :221-230

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