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Merck
  • Cyclophilin D ablation is associated with increased end-ischemic mitochondrial hexokinase activity.

Cyclophilin D ablation is associated with increased end-ischemic mitochondrial hexokinase activity.

Scientific reports (2017-10-08)
Rianne Nederlof, Mark A M van den Elshout, Anneke Koeman, Laween Uthman, Iris Koning, Otto Eerbeek, Nina C Weber, Markus W Hollmann, Coert J Zuurbier
摘要

Both the absence of cyclophilin D (CypD) and the presence of mitochondrial bound hexokinase II (mtHKII) protect the heart against ischemia/reperfusion (I/R) injury. It is unknown whether CypD determines the amount of mtHKII in the heart. We examined whether CypD affects mtHK in normoxic, ischemic and preconditioned isolated mouse hearts. Wild type (WT) and CypD-/- mouse hearts were perfused with glucose only and subjected to 25 min ischemia and reperfusion. At baseline, cytosolic and mtHK was similar between hearts. CypD ablation protected against I/R injury and increased ischemic preconditioning (IPC) effects, without affecting end-ischemic mtHK. When hearts were perfused with glucose, glutamine, pyruvate and lactate, the preparation was more stable and CypD ablation-resulted in more protection that was associated with increased mtHK activity, leaving little room for additional protection by IPC. In conclusion, in glucose only-perfused hearts, deletion of CypD is not associated with end-ischemic mitochondrial-HK binding. In contrast, in the physiologically more relevant multiple-substrate perfusion model, deletion of CypD is associated with an increased mtHK activity, possibly explaining the increased protection against I/R injury.

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Sigma-Aldrich
抗 α-微管蛋白单克隆抗体 小鼠抗, clone DM1A, ascites fluid
Sigma-Aldrich
Anti-Porin (Ab-5) (185-197) Rabbit pAb, liquid, Calbiochem®