Ischemic preconditioning affects hexokinase activity and HKII in different subcellular compartments throughout cardiac ischemia-reperfusion

doi:10.1152/japplphysiol.90537.2008

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J Appl Physiol 106: 1909-1916, 2009. First published February 19, 2009; doi:10.1152/japplphysiol.90537.2008
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	Articles by Zuurbier, C. J.

Ischemic preconditioning affects hexokinase activity and HKII in different subcellular compartments throughout cardiac ischemia-reperfusion

Ebru Gürel,¹^,3^,* Kirsten M. Smeele,¹^,* Otto Eerbeek,² Anneke Koeman,¹ Cihan Demirci,³ Markus W. Hollmann,¹ and Coert J. Zuurbier¹

Departments of ¹Anesthesiology and ²Physiology, Academic Medical Center, Amsterdam, The Netherlands; and ³Department of Biology, University of Istanbul, Istanbul, Turkey

Submitted 17 April 2008 ; accepted in final form 18 February 2009

The glycolytic enzyme hexokinase (HK) is suggested to play arole in ischemic preconditioning (IPC). In the present studywe determined how ischemic preconditioning affects HK activityand HKI and HKII protein content at five different time pointsand three different subcellular fractions throughout cardiacischemia-reperfusion. Isolated Langendorff-perfused rat hearts(10 groups of 7 hearts each) were subjected to 35 min ischemiaand 30 min reperfusion (control groups); the IPC groups werepretreated with 3 times 5-min ischemia. IPC was without effecton microsomal HK activity, and only decreased cytosolic HK activityat 35 min ischemia, which was mimicked by decreased cytosolicHKII, but not HKI, protein content. In contrast, mitochondrialHK activity at baseline and during reperfusion was elevatedby IPC, without changes during ischemia. No effect of IPC onmitochondrial HK I protein content was observed. However, mitochondrialHK II protein content during reperfusion was augmented by IPC,albeit not following the IPC stimulus. It is concluded thatIPC results in decreased cytosolic HK activity during ischemiathat could be explained by decreased HKII protein content. IPCincreased mitochondrial HK activity before ischemia and duringreperfusion that was only mimicked by increased HK II proteincontent during reperfusion. IPC was without effect on the phosphorylationstatus of HK before ischemia. We conclude that IPC is associatedwith 1) a biphasic response of increased mitochondrial HK activitybefore and after ischemia, 2) decreased cytosolic HK activityduring ischemia, and 3) cellular redistribution of HKII butnot HKI.

myocardial infarction; permeability transition pore; cardioprotection; compartmentation

Address for reprint requests and other correspondence: C. J. Zuurbier, Dept. of Anaesthesiology, Academic Medical Centre, Univ. of Amsterdam, Meibergdreef 9, 1105 AZ Amsterdam, The Netherlands (e-mail: c.j.zuurbier{at}amc.uva.nl)