A STUDY ON DILAZEP .2. DILAZEP ATTENUATES LYSOPHOSPHATIDYLCHOLINE-INDUCED MECHANICAL AND METABOLIC DERANGEMENTS IN THE ISOLATED, WORKING RAT-HEART

被引：26

作者：

HOQUE, ANE ^{[1
]}

HOQUE, N ^{[1
]}

HASHIZUME, H ^{[1
]}

ABIKO, Y ^{[1
]}

机构：

[1] ASAHIKAWA MED COLL, DEPT PHARMACOL, ASAHIKAWA 078, HOKKAIDO, JAPAN

来源：

JAPANESE JOURNAL OF PHARMACOLOGY | 1995年 / 67卷 / 03期

关键词：

DILAZEP; LYSOPHOSPHATIDYLCHOLINE; WORKING HEART; ADENOSINE TRIPHOSPHATE; FREE FATTY ACID;

D O I：

10.1254/jjp.67.233

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The effects of dilazep, d-propranolol and lidocaine on the mechanical and metabolic changes induced by lysophosphatidylcholine (LPC) were studied in isolated, perfused working rat heart. After a stabilization period, the heart was perfused for 5 min with LPC (10 mu M) alone, LPC plus dilazep (5, 10 or 20 mu M), LPC plus d-propranolol (30 or 50 mu M) or LPC plus lidocaine (30 or 100 mu M) and then perfused with normal Krebs-Henseleit bicarbonate (KHB) buffer for a further 20 min. Perfusion with LPC for 5 min followed by KHB for 20 min irreversibly decreased cardiac mechanical function, decreased the tissue levels of adenosine triphosphate and creatine phosphate significantly, and increased the tissue levels of lactate and free fatty acids including arachidonic acid. Dilazep or d-propranolol significantly attenuated the mechanical and metabolic changes induced by LPC, but lidocaine did not. These results indicate that the exogenous LPC causes ischemia-like changes, suggesting that LPC is one of the important factors in producing ischemia-reperfusion derangements in terms of mechanical and metabolic functions, and that both dilazep and d-propranolol can prevent the LPC-induced myocardial damage.

引用

页码：233 / 241

页数：9

共 38 条

[1] AUGMENTATION OF CYCLIC-AMP CONTENT INDUCED BY LYSOPHOSPHATIDYL CHOLINE IN RABBIT HEARTS [J].

AHUMADA, GG ;

BERGMANN, SR ;

CARLSON, E ;

CORR, PB ;

SOBEL, BE .

CARDIOVASCULAR RESEARCH, 1979, 13 (07) :377-382

[2]

BENTHAM JM, 1987, BASIC RES CARDIOL, V82, P127

[3] MODULATION OF CARDIAC SODIUM-CHANNEL GATING BY LYSOPHOSPHATIDYLCHOLINE [J].

BURNASHEV, NA ;

UNDROVINAS, AI ;

FLEIDERVISH, IA ;

MAKIELSKI, JC ;

ROSENSHTRAUKH, LV .

JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY, 1991, 23 :23-30

[4] ACCUMULATION OF UNESTERIFIED ARACHIDONIC-ACID IN ISCHEMIC CANINE MYOCARDIUM - RELATIONSHIP TO A PHOSPHATIDYLCHOLINE DEACYLATION-REACYLATION CYCLE AND THE DEPLETION OF MEMBRANE PHOSPHOLIPIDS [J].

CHIEN, KR ;

HAN, A ;

SEN, A ;

BUJA, LM ;

WILLERSON, JT .

CIRCULATION RESEARCH, 1984, 54 (03) :313-322

[5] MECHANISMS CONTRIBUTING TO MALIGNANT DYSRHYTHMIAS INDUCED BY ISCHEMIA IN CAT [J].

CORR, PB ;

WITKOWSKI, FX ;

SOBEL, BE .

JOURNAL OF CLINICAL INVESTIGATION, 1978, 61 (01) :109-119

[6] PATHOPHYSIOLOGICAL CONCENTRATIONS OF LYSOPHOSPHATIDES AND THE SLOW RESPONSE [J].

CORR, PB ;

SNYDER, DW ;

LEE, BI ;

GROSS, RW ;

KEIM, CR ;

SOBEL, BE .

AMERICAN JOURNAL OF PHYSIOLOGY, 1982, 243 (02) :H187-H195

[7]

CORR PB, 1981, CIRCULATION, V64, P221

[8] LYSOPHOSPHATIDYLCHOLINE-INDUCED CA2+-OVERLOAD IN ISOLATED CARDIOMYOCYTES AND EFFECT OF CYTOPROTECTIVE DRUGS [J].

DONCK, LV ;

VERELLEN, G ;

GEERTS, H ;

BORGERS, M .

JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY, 1992, 24 (09) :977-988

[9] SOLUBILIZATION AND CHARACTERIZATION OF A NEUTRAL-ACTIVE, CALCIUM-DEPENDENT, PHOSPHOLIPASE-A2 FROM RABBIT HEART AND ISOLATED CHICK-EMBRYO MYOCYTES [J].

FRANSON, RC ;

WEIR, DL ;

THAKKAR, J .

JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY, 1983, 15 (03) :189-196

[10] MECHANISMS OF ACCUMULATION OF ARACHIDONIC-ACID IN CULTURED MYOCARDIAL-CELLS DURING ATP DEPLETION [J].

GUNN, MD ;

SEN, A ;

CHANG, A ;

WILLERSON, JT ;

BUJA, LM ;

CHIEN, KR .

AMERICAN JOURNAL OF PHYSIOLOGY, 1985, 249 (06) :1188-1194

← 1 2 3 4 →