Bradykinin Protects Against Infarction but Does not Mediate Ischemic Preconditioning in the Isolated Rat Heart

Bradykinin Protects Against Infarction but Does not Mediate Ischemic Preconditioning in the Isolated Rat Heart

The aim of the study was to test if pre-ischemic treatment with bradykinin can protect against infarction in an isolated rat heart model of regional ischemia and reperfusion, and if any such protection is dependent upon activation of protein kinase C (PKC) or mediated through the nitric oxide (NO) p...

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Bibliographic Details
Published in:Journal of molecular and cellular cardiology Vol. 28; no. 12; pp. 2333 - 2341
Main Authors: Bugge, Einar, Ytrehus, Kirsti
Format: Journal Article
Language:English
Published: England Elsevier Ltd 01-12-1996
Subjects:
Animals
Bradykinin
Bradykinin - pharmacology
Chelerythrine
Heart - drug effects
Heart - physiology
Hoe 140
In Vitro Techniques
Infarct size
Ischemic preconditioning
Ischemic Preconditioning, Myocardial
Male
Myocardial Infarction - prevention & control
Nitric oxide
NOARG
Protein kinase C
Rat heart
Rats
Rats, Wistar
TTC
Protein kinase C
Hoe 140
TTC
NOARG
Bradykinin
Nitric oxide
Chelerythrine
Infarct size
Ischemic preconditioning
Rat heart
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Summary:The aim of the study was to test if pre-ischemic treatment with bradykinin can protect against infarction in an isolated rat heart model of regional ischemia and reperfusion, and if any such protection is dependent upon activation of protein kinase C (PKC) or mediated through the nitric oxide (NO) pathway. We also investigated if bradykinin B 2receptor activation, alone or in combination with activation of adenosine receptors and α-adrenoceptors, are involved in the infarct size reducing effect of ischemic preconditioning. Buffer-perfused rat hearts were subjected to 30 min regional ischemia and 120 min reperfusion. Risk zone was determined by fluorescent particles and infarct size by tetrazolium staining. Treatment with bradykinin (0.5 μmol/l) prior to ischemia significantly reduced infarct size in percentage of risk zone compared to control experiments (infarct size: 9.6±1.3% v41.8±3.6%, P<0.001). An inhibitor of NO synthesis, NOARG (100 μmol/l), did not interfere with the bradykinin induced protection (infarct size: 13.3±2.0%), while chelerythrine (2 μmol/l), an inhibitor of protein kinase C, reversed the effect of bradykinin (infarct size: 30.0±2.8%). NOARG did not influence infarct size in the control group (infarct size: 40.1±3.2%). Ischemic preconditioning with three cycles of 5 min global ischemia+5 min reperfusion offered protection similar to bradykinin (infarct size: 8.4±2.0%). The bradykinin antagonist HOE 140 (1 μmol/l) reversed the effect of bradykinin (infarct size: 42.5±3.1%), but did not interfere with ischemic preconditioning (infarct size: 7.7±1.6%). Similarily, combined blockade of α-adrenergic, adenosine and bradykinin B 2receptors with p-benzamine (10 μmol/l), SPT (100 μmol/l) and HOE 140 did not interfere with ischemic preconditioning (infarct size: 7.8±1.1%). Thus, bradykinin can protect against infarction via protein kinase C, but independently of NO. A role for bradykinin in mediating ischemic preconditioning against infarction could not be demonstrated.
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ISSN:0022-2828
1095-8584
DOI:10.1006/jmcc.1996.0226