Free Access to a Running-Wheel Advances the Phase of Behavioral and Physiological Circadian Rhythms and Peripheral Molecular Clocks in Mice

Jan 24, 2015PloS one

Access to a running wheel shifts daily behavior, body rhythms, and molecular clocks in mice

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Abstract

Voluntary wheel-running for four weeks significantly advanced the circadian phases of body temperature, food intake, and corticosterone secretion in mice.

  • Chronic voluntary exercise altered the timing of behavioral and physiological responses in mice.
  • The expression of specific was phase-advanced in the liver and white adipose tissue but not in brown adipose tissue or skeletal muscle.
  • Peak expression levels of certain clock genes increased in the skeletal muscle of mice with access to running wheels.
  • The circadian expression patterns of genes related to cholesterol and fatty acid metabolism differed significantly between sedentary and exercise conditions.

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Key numbers

Increase in Plasma Corticosterone
Corticosterone levels peaked at ZT10 in RW mice.
30 min
Circadian Phase Advancement
Onset of temperature increase was advanced by 30 minutes.

Full Text

What this is

  • This research investigates how voluntary wheel-running affects in mice.
  • Mice with access to running-wheels exhibited advanced phases in various behavioral and physiological rhythms.
  • The study analyzes changes in feeding, core body temperature, hormone levels, and gene expression related to .

Essence

  • Voluntary wheel-running in mice advanced the timing of behavioral and physiological . These changes included earlier peaks in body temperature, food intake, and hormone secretion, alongside tissue-specific alterations in clock gene expression.

Key takeaways

  • Voluntary wheel-running advanced the circadian phase of core body temperature and food intake. In running-wheel (RW) mice, the increase in body temperature started about 30 minutes earlier compared to sedentary (SED) mice.
  • Plasma corticosterone levels in RW mice peaked at ZT10 and were twice as high as in SED mice, indicating a significant hormonal response to exercise.
  • The expression of clock and clock-controlled genes was tissue-specific, with notable phase advancements in the liver and white adipose tissue of RW mice.

Caveats

  • The study does not establish causation between wheel-running and changes in . Further research is needed to clarify the mechanisms involved.
  • Findings may not be generalizable beyond the specific mouse strain and conditions used in the study.

Definitions

  • circadian rhythms: Biological processes that follow a roughly 24-hour cycle, responding primarily to light and darkness in the environment.
  • clock genes: Genes that regulate the timing of circadian rhythms through feedback loops in cellular processes.

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