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Publication : Enhanced recovery from ischemia-reperfusion injury in PI3Kα dominant negative hearts: investigating the role of alternate PI3K isoforms, increased glucose oxidation and MAPK signaling.

First Author  McLean BA Year  2013
Journal  J Mol Cell Cardiol Volume  54
Pages  9-18 PubMed ID  23142539
Mgi Jnum  J:192823 Mgi Id  MGI:5466623
Doi  10.1016/j.yjmcc.2012.10.015 Citation  McLean BA, et al. (2013) Enhanced recovery from ischemia-reperfusion injury in PI3Kalpha dominant negative hearts: investigating the role of alternate PI3K isoforms, increased glucose oxidation and MAPK signaling. J Mol Cell Cardiol 54:9-18
abstractText  Classical ischemia-reperfusion (IR) preconditioning relies on phosphatidylinositol 3-kinase (PI3K) for protective signaling. Surprisingly, inhibition of PI3Kalpha activity using a dominant negative (DN) strategy protected the murine heart from IR injury. It has been proposed that increased signaling through PI3Kgamma may contribute to the improved recovery of PI3KalphaDN hearts following IR. To investigate the mechanism by which PI3KalphaDN hearts are protected from IR injury, we created a double mutant (PI3KDM) model by crossing p110gamma(-/-) (PI3KgammaKO) with cardiac-specific PI3KalphaDN mice. The PI3KDM model has morphological and hemodynamic features that are characteristic of both PI3Kgamma(-/-) and PI3KalphaDN mice. Interestingly, when subjected to IR using ex vivo Langendorff perfusion, PI3KDM hearts showed significantly enhanced functional recovery when compared to wildtype (WT) hearts. However, signaling downstream of PI3K through Akt and GSK3beta, which has been associated with IR protection, was reduced in PI3KDM hearts. Using ex vivo working heart perfusion, we found no difference in functional recovery after IR between PI3KDM and PI3KalphaDN; also, glucose oxidation rates were significantly increased in PI3KalphaDN hearts when compared to WT, and this metabolic shift has been associated with enhanced IR recovery. However, we found that PI3KalphaDN hearts still had enhanced recovery when perfused exclusively with fatty acids (FA). We then investigated parallel signaling pathways, and found that mitogen-activated protein kinase signaling was increased in PI3KalphaDN hearts, possibly through the inhibition of negative feedback loops downstream of PI3Kalpha.
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