Uncoupling protein 3 transcription is regulated by peroxisome proliferator‐activated receptor α in the adult rodent heart

ME YOUNG, S PATIL, JUN Ying, C DEPRE… - The FASEB …, 2001 - Wiley Online Library
ME YOUNG, S PATIL, JUN Ying, C DEPRE, H SINGH AHUJA, GL SHIPLEY…
The FASEB Journal, 2001Wiley Online Library
Relatively little is known concerning the regulation of uncoupling proteins (UCPs) in the
heart. We investigated in the adult rodent heart 1) whether changes in workload, substrate
supply, or cytokine (TNF‐α) administration affect UCP‐2 and UCP‐3 ex¬ pression, and 2)
whether peroxisome proliferator‐acti¬ vated receptor α (PPARα) regulates the expression of
either UCP‐2 or UCP‐3. Direct comparisons were made between cardiac and skeletal
muscle. UCP‐2, UCP‐3, and PPARα expression were reduced when cardiac workload was …
Abstract
Relatively little is known concerning the regulation of uncoupling proteins (UCPs) in the heart. We investigated in the adult rodent heart 1) whether changes in workload, substrate supply, or cytokine (TNF‐α) administration affect UCP‐2 and UCP‐3 ex¬pression, and 2) whether peroxisome proliferator‐acti¬vated receptor α (PPARα) regulates the expression of either UCP‐2 or UCP‐3. Direct comparisons were made between cardiac and skeletal muscle. UCP‐2, UCP‐3, and PPARα expression were reduced when cardiac workload was either increased (pressure overload by aortic constriction) or decreased (mechanical unload¬ing by heterotopic transplantation). Similar results were observed during cytokine administration. Reduced di¬etary fatty acid availability resulted in decreased expres‐sion of both cardiac UCP‐2 and UCP‐3. However, when fatty acid (the natural ligand for PPARα) supply was increased (high‐fat feeding, fasting, and STZ‐induced diabetes), cardiac UCP‐3 but not UCP‐2 expression increased. Comparable results were observed in rats treated with the specific PPARα agonist WY‐14,643. The level of cardiac UCP‐3 but not UCP‐2 expression was severely reduced (20‐fold) in PPARα/ mice compared to wild‐type mice. These results suggest that in the adult rodent heart, UCP‐3 expression is regu¬lated by PPARα. In contrast, cardiac UCP‐2 expression is regulated in part by a fatty acid‐dependent, PPARα‐independent mechanism.—Young, M. E., Patil, S., Ying, J., Depre, C., Ahuja, H. S., Shipley, G. L., Stepkowski, S. M., Davies, P. J. A., Taegtmeyer H. Uncoupling protein 3 transcription is regulated by peroxisome proliferator‐activated receptor α in the adult rodent heart. FASEB J. 15, 833‐845 (2001)
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