Ranolazine increases active pyruvate dehydrogenase in perfused normoxic rat hearts: Evidence for an indirect mechanism

被引：113

作者：

Clarke, B ^{[1
]}

Wyatt, KM ^{[1
]}

McCormack, JG ^{[1
]}

机构：

[1] SYNTEX RES CTR, DEPT PHARMACOL, EDINBURGH EH14 4AP, MIDLOTHIAN, SCOTLAND

来源：

JOURNAL OF MOLECULAR AND CELLULAR CARDIOLOGY | 1996年 / 28卷 / 02期

关键词：

ranolazine; pyruvate dehydrogenase; pyruvate dehydrogenase kinase; pyruvate dehydrogenase phosphate phosphatase; metabolic modulation; mitochondria; acetyl CoA; beta-oxidation;

D O I：

10.1006/jmcc.1996.0032

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Ranolazine has shown anti-anginal efficacy in humans and cardiac anti-ischaemic activity in models, but without affecting haemodynamics or baseline contraction. In isolated normoxic rat hearts, Langendorff-perfused for 30 min with 11 mM glucose. 3% albumin, and 0.4 mM or 0.8 mM palmitate, 20 mu M ranolazine significantly increased active, dephosphorylated, pyruvate dehydrogenase (PDHa), but not with no palmitate or 1.2 mM palmitate, Dichloroactetate (DCA, 1 mM), a PDHa kinase inhibitor, significantly increased PDHa in hearts perfused with 0, 0.4 or 0.8 mar but not 1.2 mM palmitate. PDHa was significantly increased with 1.2 mM palmitate by DCA plus ranolazine, and additive effects were also seen at 0.8 mM palmitate. Activation of PDH by ranolazine and promotion of glucose oxidation offers a plausible means by which the drug may be anti-ischaemic non haemodynamically. Extensive studies with extracted enzymes and isolated rat heart mitochondria failed to demonstrate any effects of ranolazine on PDH kinase or phosphatase, or on PDH catalytic activity, whereas effects of other known effectors (such as DCA) were readily demonstrable, suggesting that ranolazine activates PDH indirectly. Further analyses of the hearts revealed that ranolazine reduced acetyl CoA content under all conditions where fatty acid was present, and +/-DCA which itself had little effect. In the absence of fatty acid, ranolazine and/or DCA raised acetyl CoA. In perfusions where octanoate (+/-albumin) replaced palmitate, ranolazine still decreased acetyl CoA, but not when acetate replaced palmitate. In octanoate-perfused hearts, the contents of the C-4, C-6 and C-8 CoA esters were all increased by ranolazine, This is consistent with ranolazine causing an inhibition of fatty acid beta-oxidation leading to decreased acetyl CoA and activation of PDH. (C) 1996 Academic Press Limited

引用

页码：341 / 350

页数：10

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