POTENTIATION OF BRADYKININ EFFECTS AND INHIBITION OF KININASE ACTIVITY IN ISOLATED SMOOTH-MUSCLE

被引：6

作者：

SCHAFFEL, R ^{[1
]}

RODRIGUES, MS ^{[1
]}

ASSREUY, J ^{[1
]}

机构：

[1] UNIV FED RIO DE JANEIRO,ICB CCS,DEPT PHARMACOL,POB 68013,BR-21944 RIO DE JANEIRO,BRAZIL

来源：

CANADIAN JOURNAL OF PHYSIOLOGY AND PHARMACOLOGY | 1991年 / 69卷 / 07期

关键词：

BRADYKININ; KININASE-II; POTENTIATION; SMOOTH MUSCLE;

D O I：

10.1139/y91-137

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Prolongation of bradykinin half-life-following kininase inhibition has been proposed as the reason for the potentiation of kinin effects. We have reassessed this assumption by using three different isolated smooth muscle preparations and simultaneously studying the inhibition of kininase activity and the potentiation of bradykinin effects by enalaprilat and BPP9a. Rat duodenum displayed higher total kininase activity, metabolizing half of the added bradykinin in 6.5 min, while this time for rat uterus was greater than 60 min. Guinea-pig ileum showed the intermediate value of 14.6 min. Enalaprilat and BPP9a slowed the metabolism of bradykinin by 50-100% in rat duodenum and by 50-180% in guinea-pig ileum, showing that a significant fraction of total kininase activity appears to be due to kininase II. In rat duodenum, an almost complete blockade of kininase activity was achieved when bacitracin and mergetpa were used together with enalaprilat. Enalaprilat and BPP9a potentiated bradykinin effects in guinea-pig ileum and rat uterus. In contrast, bradykinin-induced relaxations and contractions in rat duodenum were not potentiated by enalaprilat, BPP9a, or by the enzyme inhibitor mixture (enalaprilat - bacitracin - mergetpa). The results suggest that inhibition of bradykinin enzymatic metabolism by kininases does not necessarily lead to the potentiation of bradykinin effects.

引用

页码：904 / 908

页数：5

共 13 条

[1] FURTHER EVIDENCE FOR THE EXISTENCE OF 2 RECEPTOR-SITES FOR BRADYKININ RESPONSIBLE FOR THE DIPHASIC EFFECT IN THE RAT ISOLATED DUODENUM [J].

BOSCHCOV, P ;

PAIVA, ACM ;

PAIVA, TB ;

SHIMUTA, SI .

BRITISH JOURNAL OF PHARMACOLOGY, 1984, 83 (02) :591-600

[2] CONCENTRATIONS OF ANGIOTENSIN-CONVERTING ENZYME IN TISSUES OF RAT [J].

CUSHMAN, DW ;

CHEUNG, HS .

BIOCHIMICA ET BIOPHYSICA ACTA, 1971, 250 (01) :261-+

[3]

ERDOS EG, 1979, HDB EXPT PHARMACOLOG, V25, P428

[4] DETECTION AND ESTIMATION OF BRADYKININ IN CIRCULATING BLOOD [J].

FERREIRA, SH ;

VANE, JR .

BRITISH JOURNAL OF PHARMACOLOGY AND CHEMOTHERAPY, 1967, 29 (03) :367-&

[5]

LIEBMANN C, 1987, BIOMED BIOCHIM ACTA, V46, P469

[6] PHARMACOLOGY OF KININS - THEIR RELEVANCE TO TISSUE-INJURY AND INFLAMMATION [J].

MARCEAU, F ;

LUSSIER, A ;

REGOLI, D ;

GIROUD, JP .

GENERAL PHARMACOLOGY, 1983, 14 (02) :209-229

[7] ANGIOTENSIN-I-CONVERTING ENZYME-INHIBITOR DERIVED FROM AN ENZYMATIC HYDROLYSATE OF CASEIN .2. ISOLATION AND BRADYKININ-POTENTIATING ACTIVITY ON THE UTERUS AND THE ILEUM OF RATS [J].

MARUYAMA, S ;

NAKAGOMI, K ;

TOMIZUKA, N ;

SUZUKI, H .

AGRICULTURAL AND BIOLOGICAL CHEMISTRY, 1985, 49 (05) :1405-1409

[8]

ONDETTI MA, 1988, CIRCULATION S1, V77, P174

[9] A POTENT MERCAPTO BI-PRODUCT ANALOG INHIBITOR FOR HUMAN CARBOXYPEPTIDASE-N [J].

PLUMMER, TH ;

RYAN, TJ .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1981, 98 (02) :448-454

[10] RECEPTORS FOR BRADYKININ IN INTACT CULTURED HUMAN-FIBROBLASTS - IDENTIFICATION AND CHARACTERIZATION BY DIRECT BINDING STUDY [J].

ROSCHER, AA ;

MANGANIELLO, VC ;

JELSEMA, CL ;

MOSS, J .

JOURNAL OF CLINICAL INVESTIGATION, 1983, 72 (02) :626-635

← 1 2 →