Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms.

Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms. Research Abstract Details 

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Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms. Abstract Text:

Tak Ming Wong,Song Wu,

There is evidence that the myocytes produce dynorphin and dynorphin-like peptides, which are kappa opioid receptor (kappa-OR) agonists. Activation of kappa-OR, a dominant opioid receptor in the heart, alters the cardiac function in vivo and in vitro. The observations suggest that the endogenous kappa-opioid peptides may act as autocrines or paracrine in regulation of cardiac functions. Myocardial ischemia is a common cause of heart disorders, which is manifested in decreased myocardial performance, arrhythmia and infarct. When myocardial ischemia occurs, the sympathetic discharge increases, which in turn increases the work-load and oxygen consumption. This exacerbates the situation induced by ischemia. One of the mechanisms with which the body protects against ischemia-induced injury/arrhythmia is inhibition of stimulation of beta-adrenoceptor (beta-AR), the receptor mediating the actions of sympathetic stimulation. kappa-Opioids inhibit the beta-AR activation. The inhibition of the beta-AR activation is due to inhibition of Gs-protein and to a lesser extent the adenylyl cyclase of the signaling pathway mediating beta-AR stimulation by a pertussis sensitive G-protein that mediates kappa-OR activation. Another mechanism against ischemia-induced injury is preconditioning, which is defined as prior exposures to ischemia or other insults make the heart more tolerant to subsequent and more severe insults. Protection occurs immediately or 1-3 days after preconditioning. kappa-OR mediates protection of preconditioning with ischemia or metabolic inhibition, one of the consequences of ischemia, in the heart. Activation of kappa-OR by U50488H, a selective kappa-OR agonist (pharmacological preconditioning with U50488H, UP), activates protein kinase C (PKC), opens K(ATP) channels and increases the production of heat shock proteins. Blockade of PKC, or closing of the K(ATP) channels or inhibition of the synthesis of the heat shock protein abolishes the cardioprotection of UP. The findings indicate the important roles of PKC, the K(ATP) channels and the heat shock protein in cardioprotection of UP. In addition, UP also attenuates the Ca(2+) overload, a precipitating cause of cardiac injury, induced by ischemic insults, indicating that UP may confer cardioprotection via at least partly attenuating the Ca(2+) overload. Most interestingly, blockade of the K(ATP) channels with channel blockers, that abolishes the delayed cardioprotection of UP, also attenuates the inhibitory effect of UP on Ca(2+) overload, suggesting that the cardioprotective effect of opening of the K(ATP) channels may be due at least partly to the prevention/attenuation of Ca(2+) overload.

Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms. Publishing Authors By Initials

TM Wong,S Wu,

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Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms. Journal Published:

PUBLICATION TYPE: Journal Article

Journal: Sheng li xue bao : [Acta physiologica Sinica]

VOLUME: 55

Page Numbers: 115-20

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ISSN: 0371-0874

DAY: 25

MONTH: Apr

YEAR: 2003

Roles of kappa opioid receptors in cardioprotection against ischemia: the signaling mechanisms. Information

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LANGUAGE: eng

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AFFILIATION: Department of Physiology, The University of Hong Kong, 4/F, Laboratory Block, Faculty of Medicine Building, 21 Sassoon Road, Hong Kong SAR, China; E-mail: wongtakm@hkucc.hku.hk

Country: China

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MEDLINETA: Sheng Li Xue Bao

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