Advances in molecular biology of hibernation in mammals

Andrews, Matthew T.

doi:10.1002/bies.20560

Cited by 176 publications

(121 citation statements)

References 94 publications

(120 reference statements)

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“…The hibernation state is characterized by long periods of inactivity, depressed metabolic rate, and fasting with increased reliance on fatty acids for metabolic fuel (Andrews, 2007). Most small mammal hibernators cycle through periodic torpor bouts with a duration of 5-40 days (mean 14 days) throughout a winter season (Geiser and Ruf, 1995).…”

Section: Hibernation Backgroundmentioning

confidence: 99%

Skeletal muscle mass and composition during mammalian hibernation

Cotton

2016

Journal of Experimental Biology

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Hibernation is characterized by prolonged periods of inactivity with concomitantly low nutrient intake, conditions that would typically result in muscle atrophy combined with a loss of oxidative fibers. Yet, hibernators consistently emerge from winter with very little atrophy, frequently accompanied by a slight shift in fiber ratios to more oxidative fiber types. Preservation of muscle morphology is combined with downregulation of glycolytic pathways and increased reliance on lipid metabolism instead. Furthermore, while rates of protein synthesis are reduced during hibernation, balance is maintained by correspondingly low rates of protein degradation. Proposed mechanisms include a number of signaling pathways and transcription factors that lead to increased oxidative fiber expression, enhanced protein synthesis and reduced protein degradation, ultimately resulting in minimal loss of skeletal muscle protein and oxidative capacity. The functional significance of these outcomes is maintenance of skeletal muscle strength and fatigue resistance, which enables hibernating animals to resume active behaviors such as predator avoidance, foraging and mating immediately following terminal arousal in the spring.

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Section: Hibernation Backgroundmentioning

confidence: 99%

Skeletal muscle mass and composition during mammalian hibernation

Cotton

2016

Journal of Experimental Biology

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“…One possibility is that lowered CBT is a consequence of the reduced thyroid stimulating hormone (TSH) levels or is adaptive to the lower metabolic rate demonstrated at least in GH deficient mice [37]. No direct indication exists, to date, that the IGF-I pathway can modulate CBT, although it has been hypothesized that reduced insulin signaling may be one of the signals inducing hypothermia during hibernation [38]. Since the IGF-I pathway can regulate lifespan in poikilotherms, the insulin pathway is likely to act independently of CBT in controlling longevity and aging.…”

Section: Thermodynamic Effects and Specific Pathwaysmentioning

confidence: 99%

“…Importantly, studies on hibernation emphasized the close correlation between energy metabolism and CBT and identified some important mediators or regulators of this seasonal adaptation. These include the thyroid hormone derivative 3-iodiothyronamine, the 5'-adenosine monophosphate, the hormone grhelin and hydrogen sulfide gas, all of which are endogenous compounds that can induce hypothermia in mice (Reviewed in [38]). It is likely that further development in the field will identify molecules and pathways that are directly involved in the modulation of CBT.…”

Section: Temperature and Energy Homeostasismentioning

confidence: 99%

Considerations on Temperature, Longevity and Aging

Conti

2008

Cell. Mol. Life Sci.

105

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“…reproduction, metabolism and migration) occurs widely in the animal kingdom (Farner, 1985), yet the underlying control mechanisms remain largely unknown. Hibernation represents one of the most extreme examples of seasonal physiological adaption, which is employed by a selective subset of mammals to conserve resources in cold or inhospitable environments (Andrews, 2007;Carey et al, 2003;Drew et al, 2007;Storey, 2010). Profound and precisely-controlled physiological changes occur during hibernation, enabling these mammals to endure dramatic drops in whole-body metabolism, heart and respiratory rates, and body temperature (Carey et al, 2003;Drew et al, 2007;Hampton et al, 2010;Heldmaier et al, 2004;Storey, 2010).…”

Section: Introductionmentioning

confidence: 99%

Seasonal oscillation of liver-derived hibernation protein complex in the central nervous system of non-hibernating mammals

Seldin

Byerly

Petersen

et al. 2014

Journal of Experimental Biology

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Mammalian hibernation elicits profound changes in whole-body physiology. The liver-derived hibernation protein (HP) complex, consisting of HP-20, HP-25 and HP-27, was shown to oscillate circannually, and this oscillation in the central nervous system (CNS) was suggested to play a role in hibernation. The HP complex has been found in hibernating chipmunks but not in related nonhibernating tree squirrels, leading to the suggestion that hibernationspecific genes may underlie the origin of hibernation. Here, we show that non-hibernating mammals express and regulate the conserved homologous HP complex in a seasonal manner, independent of hibernation. Comparative analyses of cow and chipmunk HPs revealed extensive biochemical and structural conservations. These include liver-specific expression, assembly of distinct heteromeric complexes that circulate in the blood and cerebrospinal fluid, and the striking seasonal oscillation of the HP levels in the blood and CNS. Central administration of recombinant HPs affected food intake in mice, without altering body temperature, physical activity levels or energy expenditure. Our results demonstrate that HP complex is not unique to the hibernators and suggest that the HP-regulated liver-brain circuit may couple seasonal changes in the environment to alterations in physiology.

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Advances in molecular biology of hibernation in mammals

Cited by 176 publications

References 94 publications

Skeletal muscle mass and composition during mammalian hibernation

Skeletal muscle mass and composition during mammalian hibernation

Considerations on Temperature, Longevity and Aging

Seasonal oscillation of liver-derived hibernation protein complex in the central nervous system of non-hibernating mammals

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