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by Joanne S. Ingwall Circ Heart Fail Volume 2(4): July 1, 2009

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Presentation on theme: "by Joanne S. Ingwall Circ Heart Fail Volume 2(4): July 1, 2009"— Presentation transcript:

1 On the Control of Metabolic Remodeling in Mitochondria of the Failing Heart
by Joanne S. Ingwall Circ Heart Fail Volume 2(4): July 1, 2009 Copyright © American Heart Association, Inc. All rights reserved.

2 Figure. PGC-1s as master regulators of cardiac metabolism.
Figure. PGC-1s as master regulators of cardiac metabolism. Transcriptional activators and coactivators important for long-term molecular remodeling of all aspects of ATP metabolism are shown. MAT1 functions by tethering Cdk7 and cyclin H to PGC-1α, allowing transcription to occur. Each transcriptional family of activators—NRF, ERR, PPAR, RXR, and MEF-2—confer specificity of promoters targeted by PGC-1α, although there is considerable overlap. PGC-1α is activated by p38 MAPK and calcineurin A/CaMKII in response to cold, fasting and growth stimuli. Importantly, PGC-1α is lower in the failing heart. The report by Garnier et al,4 in this issue shows that ET-1 and angiotensin II downregulate whereas aldosterone and isoprenaline upregulate PGC-1α expression in ventricular myocytes. NRF indicates nuclear respiratory factors; ERR, estrogen receptors; PPAR, peroxisome proliferator-activated receptors; RXR, retinoid receptors. Joanne S. Ingwall Circ Heart Fail. 2009;2: Copyright © American Heart Association, Inc. All rights reserved.

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