Subcellular effects of myocyte-specific androgen receptor overexpression in mice

Musa, Mutaz; Fernando, Shannon M.; Chatterjee, Diptendu; Monks, D. Ashley

doi:10.1530/joe-11-0071

Cited by 15 publications

(15 citation statements)

References 53 publications

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“…We also found that fatigue resistance was reduced in the EDL, but not in the SOL, after 5 days of T treatment in Tg mice, with no effects on fatiguability at 3 days (Fig 6). Interestingly, other investigators studying the same model report that the number and size of mitochondria in the EDL increases significantly after a week of T exposure, 34 suggestive of mitochondrial dysfunction. While the EDL normally derives much of its ATP from glycolytic metabolism, the EDL from female Tgs after 9 days of T has shifted to a more oxidative metabolism based on NADH staining.…”

Section: Discussionmentioning

confidence: 85%

“…In our model, loss of muscle function is associated with both an increase in mitochondrial number and activity of complexes I, II and IV in the respiratory chain of mitochondria. 34 These mitochondrial complexes are the primary source of reactive nitrogen and oxygen. Paradoxically, the production of ATP may at the same time be decreasing, as suggested by the reduced resistance to fatigue in the EDL and a deficit in citric synthase activity found in the fast twitch muscle anterior tibialis of these same T-treated Tg mice (unpublished observation).…”

Section: Discussionmentioning

confidence: 99%

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Androgen receptors in muscle fibers induce rapid loss of force but not mass: Implications for spinal bulbar muscular atrophy

et al. 2013

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Introduction Testosterone (T) induces motor dysfunction in transgenic (Tg) mice overexpressing wild type androgen receptor (AR) in skeletal muscles. Since many genes implicated in motor neuron disease are expressed in skeletal muscles, mutant proteins may act in muscles to instigate muscle dysfunction in motor neuron disease. Methods We examined contractile properties of the extensor digitorum longus (EDL) and soleus (SOL) muscles in vitro after 5 and 3 days of T treatment in motor-impaired Tg female mice. Results Both muscles showed deficits in tetanic force after 5 days of T treatment, without losses in muscle mass, protein content, or fiber number. By 3 days of T treatment, only SOL showed a deficit in tetanic force comparable to that at 5 days of treatment. In both treatments, EDL shows slowed twitch kinetics, whereas SOL shows deficits in the twitch/tetanus ratio. Conclusions These results suggest calcium handling mechanisms in muscle fibers are defective in motor-impaired mice.

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Section: Discussionmentioning

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Androgen receptors in muscle fibers induce rapid loss of force but not mass: Implications for spinal bulbar muscular atrophy

et al. 2013

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“…For each subject, five micrographs were sampled to obtain measurements of sarcomere width (short axis) and length (long axis), mitochondrial volume density, numerical density, and mean volume were measured as described previously. Measurements of sarcomere width were performed on eight sarcomeres per photomicrograph [28]. …”

Section: Methodsmentioning

confidence: 99%

Exposure to AT1 Receptor Autoantibodies during Pregnancy Increases Susceptibility of the Maternal Heart to Postpartum Ischemia-Reperfusion Injury in Rats

Wang

Zhang

Wang

et al. 2014

IJMS

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Epidemiological studies have demonstrated that women with a history of preeclampsia have a two-fold increased risk of developing cardiovascular diseases in later life. It is not known whether or not this risk is associated with angiotensin II receptor type 1 autoantibody (AT1-AA), an agonist acting via activation of AT1 receptor (AT1R), which is believed to be involved in the pathogenesis of preeclampsia. The objective of the present study was to confirm the hypothesis that AT1-AA exposure during pregnancy may change the maternal cardiac structure and increase the susceptibility of the postpartum heart to ischemia/reperfusion injury (IRI). In the present study, we first established a preeclampsia rat model by intravenous injection of AT1-AA extracted from the plasma of rats immunized with AT1R, observed the susceptibility of the postpartum maternal heart to IRI at 16 weeks postpartum using the Langendorff preparation, and examined the cardiac structure using light and transmission electron microscopy. The modeled animals presented with symptoms very similar to the clinical symptoms of human preeclampsia during pregnancy, including hypertension and proteinuria. The left ventricular weight (LVW) and left ventricular mass index (LVMI) in AT1-AA treatment group were significantly increased as compared with those of the control group (p < 0.01), although there was no significant difference in final weight between the two groups. AT1-AA acting on AT1R not only induced myocardial cell hypertrophy, mitochondrial swelling, cristae disorganization and collagen accumulation in the interstitium but affected the left ventricular (LV) function and delayed recovery from IRI. In contrast, co-treatment with AT1-AA + losartan completely blocked AT1-AA-induced changes in cardiac structure and function. These data indicate that the presence of AT1-AA during pregnancy was strongly associated with the markers of LV geometry changes and remodeling, and increased the cardiac susceptibility to IRI in later life of postpartum maternal rats.

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“…Over-expression of AR within myocytes does indeed increase myocyte size, but curiously, it is also sufficient to decrease adipose tissue [64]. Because these alterations in body composition were associated with changes in resting metabolic rate, muscle respiration, and, in mice, alterations in mitochondrial morphology, these results are most obviously consistent with an endocrine mechanism of action [64,65]. It therefore remains possible, but it seems less likely, that endocrine mechanisms explain the effect of myocyte AR on spinal motoneurons.…”

Section: Reviewmentioning

confidence: 99%

Turning sex inside-out: Peripheral contributions to sexual differentiation of the central nervous system

2012

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Sexual differentiation of the nervous system occurs via the interplay of genetics, endocrinology and social experience through development. Much of the research into mechanisms of sexual differentiation has been driven by an implicit theoretical framework in which these causal factors act primarily and directly on sexually dimorphic neural populations within the central nervous system. This review will examine an alternative explanation by describing what is known about the role of peripheral structures and mechanisms (both neural and non-neural) in producing sex differences in the central nervous system. The focus of the review will be on experimental evidence obtained from studies of androgenic masculinization of the spinal nucleus of the bulbocavernosus, but other systems will also be considered.

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Subcellular effects of myocyte-specific androgen receptor overexpression in mice

Cited by 15 publications

References 53 publications

Androgen receptors in muscle fibers induce rapid loss of force but not mass: Implications for spinal bulbar muscular atrophy

Androgen receptors in muscle fibers induce rapid loss of force but not mass: Implications for spinal bulbar muscular atrophy

Exposure to AT1 Receptor Autoantibodies during Pregnancy Increases Susceptibility of the Maternal Heart to Postpartum Ischemia-Reperfusion Injury in Rats

Turning sex inside-out: Peripheral contributions to sexual differentiation of the central nervous system

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