Identification of the circadian transcriptome in adult mouse skeletal muscle

McCarthy, John J.; Andrews, Jessica L.; McDearmon, Erin L.; Campbell, Kenneth S.; Barber, Brigham K.; Miller, Brooke H.; Walker, John R.; Hogenesch, John B.; Takahashi, Joseph S.; Esser, Karyn A.

doi:10.1152/physiolgenomics.00066.2007

Cited by 319 publications

(328 citation statements)

References 73 publications

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“…The loss of circadian expression of MyoD in skeletal muscle from both Clock Δ19 and Bmal1 −/− mice is very similar to what has been previously observed with other genes known to be regulated by BMAL1 and CLOCK, such as Per2 and Dbp (referred to as clock-controlled genes) (7,8). Results from reporter gene assays and ChIP experiments confirmed that MyoD is a direct target of CLOCK and BMAL1.…”

Section: Discussionsupporting

confidence: 84%

“…MyoD is a wellestablished skeletal muscle-specific transcription factor that directly regulates expression of the myogenic program (9). In addition to MyoD, we found that the core components of the molecular clock, including Bmal1 and Per2 expression, were oscillating as is seen in liver and other peripheral tissues (7). Interestingly, MyoD expression, like Per2 mRNA, did not oscillate in muscle of the Clock Δ19 mutant mouse, suggesting the possibility that MyoD is a clock-controlled gene.…”

mentioning

confidence: 67%

“…To date, however, no genetic studies have examined what role circadian rhythms play in adult skeletal muscle. Our earlier results from an expression profiling study identified circadian expression of the components of the molecular clock (e.g., Bmal1, Per2) and showed that expression of MyoD, a master regulator of skeletal muscle differentiation, followed a circadian pattern (7,8).…”

Section: Discussionmentioning

confidence: 94%

“…We recently reported that myogenic differentiation 1 (MyoD) mRNA is expressed in a circadian fashion in adult skeletal muscle (7). The identification of MyoD as a circadian gene was of interest because MyoD is well-established as a master regulator of the skeletal muscle transcriptional program (9).…”

Section: Resultsmentioning

confidence: 99%

“…These mRNAs exhibit significant oscillation in gene expression with a repeating period length of 24 h. One of the intriguing observations from the array data was the finding that MyoD mRNA exhibited a circadian pattern (7,8). MyoD is a wellestablished skeletal muscle-specific transcription factor that directly regulates expression of the myogenic program (9).…”

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confidence: 99%

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CLOCK and BMAL1 regulate MyoD and are necessary for maintenance of skeletal muscle phenotype and function

Andrews

Zhang

McCarthy

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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MyoD, a master regulator of myogenesis, exhibits a circadian rhythm in its mRNA and protein levels, suggesting a possible role in the daily maintenance of muscle phenotype and function. We report that MyoD is a direct target of the circadian transcriptional activators CLOCK and BMAL1, which bind in a rhythmic manner to the core enhancer of the MyoD promoter. Skeletal muscle of Clock Δ19 and Bmal1 −/− mutant mice exhibited ∼30% reductions in normalized maximal force. A similar reduction in force was observed at the single-fiber level. Electron microscopy (EM) showed that the myofilament architecture was disrupted in skeletal muscle of Clock Δ19 , Bmal1 −/− , and MyoD −/− mice. The alteration in myofilament organization was associated with decreased expression of actin, myosins, titin, and several MyoD target genes. EM analysis also demonstrated that muscle from both Clock Δ19 and Bmal1 −/− mice had a 40% reduction in mitochondrial volume. The remaining mitochondria in these mutant mice displayed aberrant morphology and increased uncoupling of respiration. This mitochondrial pathology was not seen in muscle of MyoD −/− mice. We suggest that altered expression of both Pgc-1α and Pgc-1β in Clock Δ19 and Bmal1 −/− mice may underlie this pathology. Taken together, our results demonstrate that disruption of CLOCK or BMAL1 leads to structural and functional alterations at the cellular level in skeletal muscle. The identification of MyoD as a clock-controlled gene provides a mechanism by which the circadian clock may generate a muscle-specific circadian transcriptome in an adaptive role for the daily maintenance of adult skeletal muscle.circadian clock | myofilaments | mitochondria A fundamental, evolutionarily conserved property of most organisms, from cyanobacteria to plants and animals, is the daily cycling of their internal physiology as well as certain behaviors in animals, such as sleep and feeding (1). The timing of these circadian rhythms is synchronized to the environment by external cues, with light and nutrient availability being two of the most salient entrainment cues (2). The synchronization of endogenous circadian rhythms with the daily cycles in the environment provides an adaptive mechanism for organisms to anticipate cyclic demands on cellular physiology and behavior (3, 4). At the molecular level, the circadian clock represents a well-defined gene regulatory network composed of transcriptional-translational feedback loops (5). The positive arm of the loop is composed of the transcription factors CLOCK and BMAL1, which heterodimerize and bind to E-box elements on target genes such as Per1 to drive the negative part of the feedback loop (5). More recently, the same molecular clock factors that have been identified in the central clock in the suprachiasmatic nucleus have been found to exist in most peripheral tissues (reviewed in ref. 6).We recently characterized the circadian transcriptome of adult skeletal muscle. These mRNAs exhibit significant oscillation in gene expression with a repeating period len...

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Section: Discussionsupporting

confidence: 84%

mentioning

confidence: 67%

Section: Discussionmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

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CLOCK and BMAL1 regulate MyoD and are necessary for maintenance of skeletal muscle phenotype and function

Andrews

Zhang

McCarthy

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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319

341

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Coupled network of the circadian clocks: a driving force of rhythmic physiology

2020

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The circadian system is composed of coupled endogenous oscillators that allow living beings, including humans, to anticipate and adapt to daily changes in their environment. In mammals, circadian clocks form a hierarchically organized network with a ‘master clock’ located in the suprachiasmatic nucleus of the hypothalamus, which ensures entrainment of subsidiary oscillators to environmental cycles. Robust rhythmicity of body clocks is indispensable for temporally coordinating organ functions, and the disruption or misalignment of circadian rhythms caused for instance by modern lifestyle is strongly associated with various widespread diseases. This review aims to provide a comprehensive overview of our current knowledge about the molecular architecture and system‐level organization of mammalian circadian oscillators. Furthermore, we discuss the regulatory roles of peripheral clocks for cell and organ physiology and their implication in the temporal coordination of metabolism in human health and disease. Finally, we summarize methods for assessing circadian rhythmicity in humans.

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Genomics of the Circadian Clock

Murphy

2013

Equine Genomics

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Identification of the circadian transcriptome in adult mouse skeletal muscle

Cited by 319 publications

References 73 publications

CLOCK and BMAL1 regulate MyoD and are necessary for maintenance of skeletal muscle phenotype and function

CLOCK and BMAL1 regulate MyoD and are necessary for maintenance of skeletal muscle phenotype and function

Coupled network of the circadian clocks: a driving force of rhythmic physiology

Genomics of the Circadian Clock

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