Role of PPAR alpha in control of torpor through FGF21-NPY pathway: From circadian clock genes to seasonal change and cardiovascular disease

Norio K. Ishida
Daisuke Uchida
Ryosuke Doi
Katsutaka Oishi
Sachiko Chikahisa
Hiroyoshi Sei
Yasutaka Hamasaka
Takahiro Suzuki
Shuji Hanai

In nature, hibernating animals experience fasting, cold temperature, and short day seasonally. Torpor is a state of decreased physiological activity in an animal, usually characterized by a reduced body temperature and rate of metabolism to adapt to such a severe environment. Ablation of the central clock synchronizer, the suprachiasmatic nucleus in brain, abolishes torpor, a hibernation-like state, implicating the circadian clock involved in this seasonal change. Biologists know well that the energy source of daily heterotherms/hibernators change from glucose to lipids in winter. Here we review several lines of evidence of a master transcriptional regulator in lipid catabolism, peroxisome proliferator-activated receptor alpha (PPAR alpha), in the control of torpor through the fibroblast growth factor 21-neuropeptide Y (FGF21-NPY) pathway. 1 Furthermore, we showed the role of PERIOD2 protein as a suppressor of plasminogen activator inhibitor-1(PAI-1) gene expression using PER2 transgenic mice. These indicates the importance of clock genes to tell seasons to improve and cardiovascular function.

SLEEP AND BIOLOGICAL RHYTHMS

WILEY-BLACKWELL PUBLISHING, INC

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10.1111/j.1479-8425.2009.00413.x

https://doi.org/10.1111/j.1479-8425.2009.00413.x
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