Voluntary Wheel Running Attenuates Muscle Mass And Myosin Isoform Changes In Cancer Cachexia

After 14 generations of selection for voluntary wheel running, mice from the four replicate selected lines ran, on average, twice as many revolutions per day as those from the four unselected control lines. To examine whether the selected lines followed distinct strategies in the correlated responses of the size and metabolic capacities of the hindlimb muscles, we examined mice from selected lines, housed for 8 wk in cages with access to running wheels that were either free to rotate (“wheel access” group) or locked (“sedentary”). Thirteen of twenty individuals in one selected line (line 6) and two of twenty in another (line 3) showed a marked reduction (∼50%) in total hindlimb muscle mass, consistent with the previously described expression of a small-muscle phenotype. Individuals with these “mini-muscles” were not significantly smaller in total body mass compared with line-mates with normal-sized muscles. Access to free wheels did not affect the relative mass of the mini-muscles, but did result in typical mammalian training effects for mitochondrial enzyme activities. Individuals with mini-muscles showed a higher mass-specific muscle aerobic capacity as revealed by the maximal in vitro rates of citrate synthase and cytochrome c oxidase. Moreover, these mice showed the highest activities of hexokinase and carnitine palmitoyl transferase. Females with mini-muscles showed the highest levels of phosphofructokinase, and males with mini-muscles the highest levels of pyruvate dehydrogenase. As shown by total muscle enzyme contents, the increase in mass-specific aerobic capacity almost completely compensated for the reduction caused by the “loss” of muscle mass. Moreover, the mini-muscle mice exhibited the lowest contents of lactate dehydrogenase and glycogen phosphorylase. Interestingly, metabolic capacities of mini-muscled mice resemble those of muscles after endurance training. Overall, our results demonstrate that during selection for voluntary wheel running, distinct adaptive paths that differentially exploit the genetic variation in morphological and physiological traits have been followed.

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Voluntary running, skeletal muscle gene expression, and signaling inversely regulated by orchidectomy and testosterone replacement

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00402.2010 ◽

2011 ◽

Vol 300 (2) ◽

pp. E327-E340 ◽

Cited By ~ 59

Author(s):

Chikwendu Ibebunjo ◽

John K. Eash ◽

Christine Li ◽

QiCheng Ma ◽

David J. Glass

Keyword(s):

Skeletal Muscle ◽

Muscle Mass ◽

Wheel Running ◽

Natural Aging ◽

Testosterone Replacement ◽

Muscle Size ◽

High Dose ◽

Voluntary Wheel Running ◽

E3 Ligases ◽

Voluntary Wheel

Declines in skeletal muscle size and strength, often seen with chronic wasting diseases, prolonged or high-dose glucocorticoid therapy, and the natural aging process in mammals, are usually associated with reduced physical activity and testosterone levels. However, it is not clear whether the decline in testosterone and activity are causally related. Using a mouse model, we found that removal of endogenous testosterone by orchidectomy results in an almost complete cessation in voluntary wheel running but only a small decline in muscle mass. Testosterone replacement restored running behavior and muscle mass to normal levels. Orchidectomy also suppressed the IGF-I/Akt pathway, activated the atrophy-inducing E3 ligases MuRF1 and MAFBx, and suppressed several energy metabolism pathways, and all of these effects were reversed by testosterone replacement. The study also delineated a distinct, previously unidentified set of genes that is inversely regulated by orchidectomy and testosterone treatment. These data demonstrate the necessity of testosterone for both speed and endurance of voluntary wheel running in mice and suggest a potential mechanism for declined activity in humans where androgens are deficient.

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Therapeutic effects of voluntary wheel running on cardiac dysfunction induced by cancer cachexia

Proceedings for Annual Meeting of The Japanese Pharmacological Society ◽

10.1254/jpssuppl.wcp2018.0_po3-3-8 ◽

2018 ◽

Vol WCP2018 (0) ◽

pp. PO3-3-8

Author(s):

Susumu Ueno ◽

Miki Nonaka ◽

Ryo Kakigi ◽

Nagomi Kurebayashi ◽

Takashi Murayama ◽

...

Keyword(s):

Cardiac Dysfunction ◽

Cancer Cachexia ◽

Wheel Running ◽

Therapeutic Effects ◽

Voluntary Wheel Running ◽

Voluntary Wheel

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Maximal oxygen consumption in relation to subordinate traits in lines of house mice selectively bred for high voluntary wheel running

Journal of Applied Physiology ◽

10.1152/japplphysiol.00042.2006 ◽

2006 ◽

Vol 101 (2) ◽

pp. 477-485 ◽

Cited By ~ 44

Author(s):

Enrico L. Rezende ◽

Fernando R. Gomes ◽

Jessica L. Malisch ◽

Mark A. Chappell ◽

Theodore Garland

Keyword(s):

Muscle Mass ◽

Citrate Synthase ◽

Wheel Running ◽

Maximal Oxygen Consumption ◽

Hemoglobin Concentration ◽

Cellular Respiration ◽

Voluntary Wheel Running ◽

Hindlimb Muscle ◽

The Individual ◽

Voluntary Wheel

We studied relations between maximal O2 consumption (V̇o2 max) during forced exercise and subordinate traits associated with blood O2 transport and cellular respiration in four lines of mice selectively bred for high voluntary wheel running (S lines) and their four nonselected control (C) lines. Previously, we reported V̇o2 max of 59 females at three Po2 (hypoxia = 14% O2, normoxia = 21%, hyperoxia = 30%). Here, we test the hypothesis that variation in V̇o2 max can be explained, in part, by hemoglobin concentration and Po2 necessary to obtain 50% O2 saturation of Hb (an estimate of Hb affinity for O2) of the blood as well as citrate synthase activity and myoglobin concentration of ventricles and gastrocnemius muscle. Statistical analyses controlled for body mass, compared S and C lines, and also considered effects of the mini-muscle phenotype (present only in S lines and resulting from a Mendelian recessive allele), which reduces hindlimb muscle mass while increasing muscle mass-specific aerobic capacity. Although S lines had higher V̇o2 max than C, subordinate traits showed no statistical differences when the presence of the mini-muscle phenotype was controlled. However, subordinate traits did account for some of the individual variation in V̇o2 max. Ventricle size was a positive predictor of V̇o2 max at all three Po2. Blood Hb concentration was a positive predictor of V̇o2 max in S lines but a negative predictor in C lines, indicating that the physiological underpinnings of V̇o2 max have been altered by selective breeding. Mice with the mini-muscle phenotype had enlarged ventricles, with higher mass-specific citrate synthase activity and myoglobin concentration, which may account for their higher V̇o2 max in hypoxia.

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