期刊
CELL METABOLISM
卷 19, 期 2, 页码 319-330出版社
CELL PRESS
DOI: 10.1016/j.cmet.2013.12.016
关键词
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资金
- Israel Science Foundation (ISF)
- Abish-Frenkel Foundation
- HFSP Career Development Award [HFSP CDA00014/2012]
- European Research Council [ERC-2011 METACYCLES 310320]
- National Institute on Aging [R01 AG31675]
- Feinberg Graduate School, Weizmann Institute of Science
- intramural institutional research funds
Circadian clocks play a major role in orchestrating daily physiology, and their disruption can evoke metabolic diseases such as fatty liver and obesity. To study the role of circadian clocks in lipid homeostasis, we performed an extensive lipidomic analysis of liver tissues from wild-type and clock-disrupted mice either fed ad libitum or night fed. To our surprise, a similar fraction of lipids (similar to 17%) oscillated in both mouse strains, most notably triglycerides, but with completely different phases. Moreover, several master lipid regulators (e. g., PPAR alpha) and enzymes involved in triglyceride metabolism retained their circadian expression in clock-disrupted mice. Nighttime restricted feeding shifted the phase of triglyceride accumulation and resulted in similar to 50% decrease in hepatic triglyceride levels in wild-type mice. Our findings suggest that circadian clocks and feeding time dictate the phase and levels of hepatic triglyceride accumulation; however, oscillations in triglycerides can persist in the absence of a functional clock.
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