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1. Deciphering the Role of Proteoglycans and Glycosaminoglycans in Health and Disease.

Author

Debruin, Danielle, McRae, Natasha L., Addinsall, Alex B., McCulloch, Daniel R., Barker, Robert G., Debrincat, Didier, Hayes, Alan, Murphy, Robyn M., and Stupka, Nicole

Subjects
DUCHENNE muscular dystrophy, RESPIRATORY muscles, EXTRACELLULAR matrix, GLYCOSAMINOGLYCANS, PROTEOGLYCANS, SOLEUS muscle, HINDLIMB
Abstract

Versican is increased with inflammation and fibrosis, and is upregulated in Duchenne muscular dystrophy. In fibrotic diaphragm muscles from dystrophic mdx mice, genetic reduction of versican attenuated macrophage infiltration and improved contractile function. Versican is also implicated in myogenesis. Here, we investigated whether versican modulated mdx hindlimb muscle pathology, where inflammation and regeneration are increased but fibrosis is minimal. Immunohistochemistry and qRT-PCR were used to assess how fiber type and glucocorticoids (α-methylprednisolone) modify versican expression. To genetically reduce versican, female mdx and male versican haploinsufficient (hdf) mice were bred resulting in male mdx-hdf and mdx (control) pups. Versican expression, contractile function, and pathology were evaluated in hindlimb muscles. Versican immunoreactivity was greater in slow versus fast hindlimb muscles. Versican mRNA transcripts were reduced by α-methylprednisolone in soleus, but not in fast extensor digitorum longus, muscles. In juvenile (6-wk-old) mdx-hdf mice, versican expression was most robustly decreased in soleus muscles leading to improved force output and a modest reduction in fatiguability. These functional benefits were not accompanied by decreased inflammation. Muscle architecture, regeneration markers, and fiber type also did not differ between mdx-hdf mice and mdx littermates. Improvements in soleus contractile function were not retained in adult (20-wk-old) mdx-hdf mice. In conclusion, soleus muscles from juvenile mdx mice were most responsive to pharmacological or genetic approaches targeting versican; however, the benefits of versican reduction were limited due to low fibrosis. Preclinical matrix research in dystrophy should account for muscle phenotype (including age) and the interdependence between inflammation and fibrosis. [ABSTRACT FROM AUTHOR]

Published
2024
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2. Tiny changes in cytoplasmic [Ca2+] cause large changes in mitochondrial Ca2+: what are the triggers and functional implications?

Author

Crystal Seng, Luke Pearce, Aldo Meizoso-Huesca, Daniel P. Singh, Robyn M. Murphy, Cedric R. Lamboley, and Bradley S. Launikonis

Subjects
Physiology, Cell Biology
Abstract

Ca2+ is an integral component of the functional and developmental regulation of the mitochondria. In skeletal muscle, Ca2+ is reported to modulate the rate of ATP resynthesis, regulate the expression of peroxisome proliferator-activated receptor-gamma coactivator 1 (PGC1α) following exercise, and drive the generation of reactive oxygen species (ROS). Due to the latter, mitochondrial Ca2+ overload is recognized as a pathophysiological event but the former events represent important physiological functions in need of tight regulation. Recently, we described the relationship between [Ca2+]mito and resting [Ca2+]cyto and other mitochondrial Ca2+-handling properties of skeletal muscle. An important next step is to understand the triggers for Ca2+ redistribution between intracellular compartments, which determine the mitochondrial Ca2+ load. These triggers in both physiological and pathophysiological scenarios can be traced to the coupled activity of the ryanodine receptor 1 (RyR1) and store-operated Ca2+ entry (SOCE) in the resting muscle. In this piece, we will discuss some issues regarding Ca2+ measurements relevant to mitochondrial Ca2+-handling, the steady-state relationship between cytoplasmic and mitochondrial Ca2+, and the potential implications for Ca2+ handling by muscle mitochondria and cellular function.

Published
2022

3. Muscle fiber type-specific autophagy responses following an overnight fast and mixed meal ingestion in human skeletal muscle

Author

María G. Morales-Scholz, Stefan G. Wette, Jayden R. Stokie, Bianca T. Tepper, Courtney Swinton, David L. Hamilton, Karen M. Dwyer, Robyn M. Murphy, Kirsten F. Howlett, and Christopher S. Shaw

Subjects
Male, Eating, Physiology, Physiology (medical), Endocrinology, Diabetes and Metabolism, Muscle Fibers, Skeletal, Autophagosomes, Autophagy, Humans, Muscle, Skeletal
Abstract

The aim of the present study was to investigate the fiber type-specific abundance of autophagy-related proteins after an overnight fast and following ingestion of a mixed meal in human skeletal muscle. Twelve overweight, healthy young male volunteers underwent a 3-h mixed meal tolerance test following an overnight fast. Blood samples were collected in the overnight-fasted state and throughout the 180-min postmeal period. Skeletal muscle biopsies were collected in the fasted state, and at 30 and 90 min after meal ingestion. Protein content of key autophagy markers and upstream signaling responses were measured in whole muscle and pooled single fibers using immunoblotting. In the fasted state, type I fibers displayed lower LC3B-I but higher LC3B-II abundance and higher LC3B-II/LC3B-I ratio compared with type II fibers (

Published
2022

6. Impact of exercise training status on the fiber type-specific abundance of proteins regulating intramuscular lipid metabolism

Author

Christopher S. Shaw, Tasman Erftemeyer, Maria G Morales-Scholz, Andrew Aldous, Natasha L. McRae, Courtney Swinton, Robyn M. Murphy, and Kirsten F. Howlett

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, Physiology, Biology, 03 medical and health sciences, Oxygen Consumption, 0302 clinical medicine, Physiology (medical), Lipid droplet, Internal medicine, medicine, Humans, Muscle, Skeletal, Exercise, Fiber type, Athletes, Skeletal muscle, Lipid metabolism, 030229 sport sciences, Lipid Metabolism, biology.organism_classification, Muscle Fibers, Slow-Twitch, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Physical Endurance
Abstract

Endurance training enhances the capacity for fat oxidation during exercise due to increased utilization of intramuscular lipid (IMCL). This study quantitatively investigated the impact of exercise training status on muscle fiber type-specific abundance of regulatory proteins involved in IMCL utilization. Endurance-trained [ n = 7 subjects, peak oxygen consumption (V̇o2peak) 62.6 ± 4.1 (SD) mL·min−1·kg−1] and non-endurance-trained ( n = 8 subjects, V̇o2peak 44.9 ± 5.3 mL·min−1·kg−1) young men completed an incremental exercise test to determine maximal fat oxidation (MFO) and maximal oxygen uptake. Fiber type-specific IMCL content and protein abundance were assessed with immunofluorescence microscopy and immunoblot analysis of pooled single muscle fibers and whole muscle. Endurance-trained individuals displayed a higher MFO rate (0.45 ± 0.15 vs. 0.19 ± 0.07 g/min, P < 0.05), a greater proportion of type I muscle fibers, and higher IMCL content compared with untrained individuals ( P < 0.05). Adipose triglyceride lipase, hormone-sensitive lipase, perilipin 2, perilipin 5, and hydroxyacyl-coenzyme A dehydrogenase abundances were ~2–3-fold higher in type I muscle fibers compared with type IIa fibers ( P < 0.05). Correspondingly, these lipid proteins and oxidative enzymes were higher in endurance-trained individuals when assessed in whole muscle. MFO rate was strongly related to the proportion of type I fibers ( R = 0.81, P < 0.01). The abundance of proteins involved in the regulation of IMCL storage and oxidation is highly muscle fiber type specific. The increased capacity for fat oxidation in endurance-trained individuals corresponded with increased IMCL content and elevated abundance of lipolytic and oxidative enzymes in combination with a greater proportion of type I muscle fibers. NEW & NOTEWORTHY We have utilized contemporary techniques to compare the fiber type-specific characteristics of skeletal muscle from endurance-trained athletes and untrained individuals. We show that type I muscle fibers have a coordinated upregulation of proteins controlling intramuscular lipid storage, mobilization, and oxidation. Furthermore, the enhanced capacity for intramuscular lipid storage and utilization in endurance-trained individuals is related to the increased expression of lipid regulatory proteins combined with a greater proportion of type I muscle fibers.

Published
2020

7. Tiny changes in cytoplasmic [Ca2+] cause large changes in mitochondrial Ca2+: what are the triggers and functional implications?

Author

Seng, Crystal, Pearce, Luke, Meizoso-Huesca, Aldo, Singh, Daniel P., Murphy, Robyn M., Lamboley, Cedric R., and Launikonis, Bradley S.

Subjects
RYANODINE receptors, PEROXISOME proliferator-activated receptors, MITOCHONDRIA, CELL physiology, REACTIVE oxygen species, SKELETAL muscle
Abstract

Ca2+ is an integral component of the functional and developmental regulation of the mitochondria. In skeletal muscle, Ca2+ is reported to modulate the rate of ATP resynthesis, regulate the expression of peroxisome proliferator-activated receptor-gamma coactivator 1 (PGC1a) following exercise, and drive the generation of reactive oxygen species (ROS). Due to the latter, mitochondrial Ca2+ overload is recognized as a pathophysiological event but the former events represent important physiological functions in need of tight regulation. Recently, we described the relationship between [Ca2+]mito and resting [Ca2+]cyto and other mitochondrial Ca2+-handling properties of skeletal muscle. An important next step is to understand the triggers for Ca2+ redistribution between intracellular compartments, which determine the mitochondrial Ca2+ load. These triggers in both physiological and pathophysiological scenarios can be traced to the coupled activity of the ryanodine receptor 1 (RyR1) and store-operated Ca2+ entry (SOCE) in the resting muscle. In this piece, we will discuss some issues regarding Ca2+ measurements relevant to mitochondrial Ca2+-handling, the steady-state relationship between cytoplasmic and mitochondrial Ca2+, and the potential implications for Ca2+ handling by muscle mitochondria and cellular function. [ABSTRACT FROM AUTHOR]

Published
2022
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8. Upregulation of store-operated [Ca.sup.2+] entry in dystrophic mdx mouse muscle

Author

Edwards, Joshua N., Friedrich, Oliver, Cully, Tanya R., von Wegner, Frederic, Murphy, Robyn M., and Launikonis, Bradley S.

Subjects
Muscles -- Research, Sarcoplasmic reticulum -- Properties, Muscular dystrophy -- Research, Biological sciences
Abstract

Store-operated [Ca.sup.2+] entry (SOCE) is an important mechanism in virtually all cells. In adult skeletal muscle, this mechanism is highly specialized for the rapid delivery of [Ca.sup.2+] from the transverse tubule into the junctional cleft during periods of depleting [Ca.sup.2+] release. In dystrophic muscle fibers, SOCE may be a source of [Ca.sup.2+] overload, leading to cell necrosis. However, this possibility is yet to be examined in an adult fiber during [Ca.sup.2+] release. To examine this, [Ca.sup.2+] in the tubular system and cytoplasm were simultaneously imaged during direct release of [Ca.sup.2+] from sarcoplasmic reticulum (SR) in skeletal muscle fibers from healthy (wild-type, WT) and dystrophic mdx mouse. The mdx fibers were found to have normal activation and deactivation properties of SOCE. However, a depression of the cytoplasmic [Ca.sup.2+] transient in mdx compared with WT fibers was observed, as was a shift in the SOCE activation and deactivation thresholds to higher SR [Ca.sup.2+] concentrations ([[[Ca.sup.2+]].sub.SR]). The shift in SOCE activation and deactivation thresholds was accompanied by an approximately threefold increase in STIM1 and Orail proteins in dystrophic muscle. While the mdx fibers can introduce more [Ca.sup.2+] into the fiber for an equivalent depletion of [[[Ca.sup.2+]].sub.SR] via SOCE, it remains unclear whether this is deleterious. skeletal muscle; sarcoplasmic reticulum; muscular dystrophy; STIM1; Orail; excitation-contraction coupling doi: 10.1152/ajpcell.00524.2009.

Published
2010

9. Involvement of calpains in [Ca.sup.2+]-induced disruption of excitation-contraction coupling in mammalian skeletal muscle fibers

Author

Verburg, Esther, Murphy, Robyn M., Richard, Isabelle, and Lamb, Graham D.

Subjects
Calpain -- Physiological aspects, Calpain -- Research, Muscle contraction -- Research, Muscle proteins -- Physiological aspects, Muscle proteins -- Research, Biological sciences
Abstract

In skeletal muscle fibers, the coupling between excitation of the surface membrane and the release of [Ca.sup.2+] from the sarcoplasmic reticulum is irreversibly disrupted if cytoplasmic [Ca.sup.2+] concentration ([[Ca.sup.2+]]) is raised to micromolar levels for a prolonged period. This excitation-contraction (EC) uncoupling may contribute to muscle weakness after some types of exercise and in certain muscle diseases and has been linked to structural alteration of the triad junctions, but its molecular basis is unclear. Both [mu]-calpain, a ubiquitous [Ca.sup.2+]-activated protease, and muscle-specific calpain-3 become autolytically activated at micromolar [Ca.sup.2+] and have been suggested to be responsible for the uncoupling. This study used controlled [Ca.sup.2+] exposure in mechanically skinned fibers from extensor digitorum longus muscle to show that EC uncoupling still occurs in muscle fibers of calpain-3-deficient mice, with a [Ca.sup.2+] dependence indistinguishable from that in normal mice and rats. Western blotting of muscle fibers that had been partially EC uncoupled by exposure to an intermediate [Ca.sup.2+] level (~5 [micro]M [Ca.sup.2+] for 3 rain, no ATP) showed the presence of autolytic activation of a proportion of the [mu]-calpain present, but with little or no activation of calpain-3. Homogenates of normal and calpain-3-deficient muscles exposed to micromolar [Ca.sup.2+] displayed similar levels of diffusible proteolytic activity, as gauged by the rate of decline of passive force in stretched, skinned muscle fibers. Exogenously added [mu]-calpain, preactivated by elevated [[Ca.sup.2+]] and applied in the presence of 1 [micro]M [Ca.sup.2+], disrupted EC coupling in a manner similar to raised [[Ca.sup.2+]]. We conclude that calpain-3 is not responsible for [Ca.sup.2+]-induced disruption of EC coupling, but that [mu]-calpain is a plausible candidate. calpain-3; [mu]-calpain; skinned fiber; muscle fatigue; knockout mice

Published
2009

12. Abundance of ClC-1 chloride channel in human skeletal muscle: fiber type specific differences and effect of training

Author

Thomas P. Gunnarsson, Martin Thomassen, Jens Bangsbo, Casper Skovgaard, Peter M. Christensen, Morten Hostrup, Brett A. Cromer, and Robyn M. Murphy

Subjects
Adult, Male, 0301 basic medicine, Physiology, Single fiber, Single fibre, Protein expression, Contractility, 03 medical and health sciences, Oxygen Consumption, 0302 clinical medicine, Chloride Channels, Abundance (ecology), Physiology (medical), medicine, Humans, Exercise, Fiber type, urogenital system, Chemistry, Skeletal muscle, Muscle Fibers, Slow-Twitch, 030104 developmental biology, medicine.anatomical_structure, Muscle Fibers, Fast-Twitch, Chloride channel, Biophysics, Female, 030217 neurology & neurosurgery, Muscle Contraction
Abstract

Cl−channel protein 1 (ClC-1) may be important for excitability and contractility in skeletal muscle, but ClC-1 abundance has not been examined in human muscle. The aim of the present study was to examine ClC-1 abundance in human skeletal muscle, including fiber type specific differences and the effect of exercise training. A commercially available antibody was tested with positive and negative control tissue, and it recognized specifically ClC-1 in the range from 100 to 150 kDa. Abundance of ClC-1 was 38% higher ( P < 0.01) in fast twitch Type IIa muscle fibers than in slow twitch Type I. Muscle ClC-1 abundance did not change with 4 wk of training consisting of 30 min cycling at 85% of maximal heart rate (HRmax) and 3 × 30-s all out sprints or during a 7-wk training period with 10–12 × 30 s uphill cycling and 4–5 × ~4 min cycling at 90%–95% of HRmax. ClC-1 abundance correlated negatively ( P < 0.01) with maximal oxygen consumption ( r = –0.552) and incremental exercise performance ( r = –0.546). In addition, trained cyclists had lower ( P < 0.01) ClC-1 abundance than lesser trained individuals. The present observations indicate that a low abundance of muscle ClC-1 may be beneficial for exercise performance, but the role of abundance and regulation of ClC-1 in skeletal muscle of humans with respect to exercise performance and trainability need to be elucidated.NEW & NOTEWORTHY Abundance of the Cl−channel protein 1 (ClC-1) chloride channel may be important for excitability and contractility in human skeletal muscle and may therefore have implications for fatigue development. In this study, we confirmed ClC-1 specificity for a commercially available antibody, and this study is first to our knowledge to determine ClC-1 protein abundance in human muscle by Western blotting. We observed that abundance of ClC-1 was higher in fast compared with slow twitch fibers and lower in trained individuals than in recreationally active.

Published
2018

13. Cold-water immersion after training sessions: effects on fiber type-specific adaptations in muscle K+transport proteins to sprint-interval training in men

Author

James R. Broatch, Robyn M. Murphy, Danny Christiansen, Michael J. McKenna, David Bishop, and Jens Bangsbo

Subjects
medicine.medical_specialty, Fiber type, Physiology, business.industry, 030204 cardiovascular system & hematology, Interval training, 03 medical and health sciences, 0302 clinical medicine, Physical medicine and rehabilitation, Sprint, Human muscle, Water immersion, Physiology (medical), medicine, business, 030217 neurology & neurosurgery, Fibre type
Abstract

Effects of regular use of cold-water immersion (CWI) on fiber type-specific adaptations in muscle K+transport proteins to intense training, along with their relationship to changes in mRNA levels after the first training session, were investigated in humans. Nineteen recreationally active men (24 ± 6 yr, 79.5 ± 10.8 kg, 44.6 ± 5.8 ml·kg−1·min−1) completed six weeks of sprint-interval cycling, either without (passive rest; CON) or with training sessions followed by CWI (15 min at 10°C; COLD). Muscle biopsies were obtained before and after training to determine abundance of Na+, K+-ATPase isoforms (α1–3, β1–3) and phospholemman (FXYD1) and after recovery treatments (+0 h and +3 h) on the first day of training to measure mRNA content. Training increased ( P < 0.05) the abundance of α1and β3in both fiber types and β1in type-II fibers and decreased FXYD1 in type-I fibers, whereas α2and α3abundance was not altered by training ( P > 0.05). CWI after each session did not influence responses to training ( P > 0.05). However, α2mRNA increased after the first session in COLD (+0 h, P < 0.05) but not in CON ( P > 0.05). In both conditions, α1and β3mRNA increased (+3 h; P < 0.05) and β2mRNA decreased (+3 h; P < 0.05), whereas α3, β1, and FXYD1 mRNA remained unchanged ( P > 0.05) after the first session. In summary, Na+,K+-ATPase isoforms are differently regulated in type I and II muscle fibers by sprint-interval training in humans, which, for most isoforms, do not associate with changes in mRNA levels after the first training session. CWI neither impairs nor improves protein adaptations to intense training of importance for muscle K+regulation.NEW & NOTEWORTHY Although cold-water immersion (CWI) after training and competition has become a routine for many athletes, limited published evidence exists regarding its impact on training adaptation. Here, we show that CWI can be performed regularly without impairing training-induced adaptations at the fiber-type level important for muscle K+handling. Furthermore, sprint-interval training invoked fiber type-specific adaptations in K+transport proteins, which may explain the dissociated responses of whole-muscle protein levels and K+transport function to training previously reported.

Published
2018

14. Mitochondrial content is preserved throughout disease progression in the mdx mouse model of Duchenne muscular dystrophy, regardless of taurine supplementation

Author

Robert G. Barker, Robyn M. Murphy, Victoria L. Wyckelsma, and Hongyang Xu

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, mdx mouse, Weakness, Taurine, Time Factors, Physiology, Duchenne muscular dystrophy, Citrate (si)-Synthase, Mitochondrion, Mitochondrial Dynamics, GTP Phosphohydrolases, Electron Transport Complex IV, Mitochondrial Proteins, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, medicine, Animals, Muscle, Skeletal, Wasting, Electron Transport Complex I, biology, business.industry, Membrane Proteins, Skeletal muscle, Cell Biology, musculoskeletal system, medicine.disease, Mitochondria, Muscle, Mice, Inbred C57BL, Muscular Dystrophy, Duchenne, Disease Models, Animal, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, chemistry, Dietary Supplements, Disease Progression, Mice, Inbred mdx, biology.protein, medicine.symptom, Dystrophin, business, tissues, 030217 neurology & neurosurgery
Abstract

Mitochondrial dysfunction is a pathological feature of Duchenne muscular dystrophy (DMD), a debilitating and fatal neuromuscular disorder characterized by progressive muscle wasting and weakness. Mitochondria are a source of cellular ATP involved in Ca2+ regulation and apoptotic signaling. Ameliorating aberrant mitochondrial function has therapeutic potential for reducing DMD disease severity. The dystrophic mdx mouse exhibits peak muscle damage at 21–28 days, which stabilizes after 8 wk. The amino acid taurine is implicated in mitochondrial health and function, with endogenous concentrations low when measured during the cycle of peak muscle damage in mdx mice. Using whole soleus and extensor digitorum longus (EDL) muscle homogenates from 28- and 70-day mdx mice, we found that there was no change in native state mitochondrial complexes using blue native-PAGE. NADH:ubiquinone oxidotreductase subunit-A9 (NDUFA9) protein abundance was lower in soleus muscle of 28- and 70-day mdx mice and EDL muscle of 70-day mdx mice compared with same muscles in WT (C57/BL10ScSn) animals. There were age-dependent increases in both NDUFA9 protein abundance and citrate synthase activity in soleus muscles of mdx and wild-type mice. There was no change in abundances of mitochondrial dynamics proteins mitofusin 2 (Mfn2) and mitochondrial dynamics protein 49 (MiD49). Taurine administration essentially did not affect any measurements of mitochondria. Collectively, these findings suggest mitochondrial content and dynamics are not reduced in the mdx mouse regardless of disease severity. We also elucidate that taurine affords no significant benefit to mitochondrial content or dynamics in the mdx mouse at either 28 or 70 days.

Published
2018

15. [micro]-Calpain and calpain-3 are not autolyzed with exhaustive exercise in humans

Author

Murphy, Robyn M., Snow, Rodney J., and Lamb, Graham D.

Subjects
Proteolysis -- Research, Calpain -- Research, Biological sciences
Abstract

[micro]-calpain and calpain-3 are [Ca.sup.2+]+-dependent proteases found in skeletal muscle. Autolysis of calpains is observed using Western blot analysis as the cleaving of the full-length proteins to shorter products. Biochemical assays suggest that [micro]-calpain becomes proteolytically active in the presence of 2-200 [micro]M [Ca.sup.2+]. Although calpain-3 is poorly understood, autolysis is thought to result in its activation, which is widely thought to occur at lower intracellular [Ca.sup.2+] concentration levels ([[[Ca.sup.2+]].sub.i]; -1 [micro]M) than the levels at which [micro]-calpain activation occurs. We have demonstrated the [Ca.sup.2+]-dependent autolysis of the calpains in human muscle samples and rat extensor digitorum longus (EDL) muscles homogenized in solutions mimicking the intracellular environment at various [[Ca.sup.2+]] levels (0, 2.5, 10, and 25 [micro]M). Autolysis of calpain-3 was found to occur across a [[Ca.sup.2+]] range similar to that for [micro]-calpain, and both calpains displayed a seemingly higher [Ca.sup.2+] sensitivity in human than in rat muscle homogenates, with ~15% autolysis observed after 1-min exposure to 2.5 [micro]M [Ca.sup.2+] in human muscle and almost none after 1- to 2-min exposure to the same [[[Ca.sup.2+]].sub.i] level in rat muscle. During muscle activity, [[[Ca.sup.2+]].sub.i] may transiently peak in the range found to autolyze [micro]-calpain and calpain-3, so we examined the effect of two types of exhaustive cycling exercise (30-s 'all-out' cycling, n = 8; and 70% V[O.sub.2] peak until fatigue, n = 3) on the amount of autolyzed po-calpain or calpain-3 in human muscle. No significant autolysis of [micro]-calpain or calpain-3 occurred as a result of the exercise. These findings have shown that the time- and concentration-dependent changes in [[[Ca.sup.2+]].sub.i] that occurred during concentric exercise fall near but below the level necessary to cause autolysis of calpains in vivo. [Ca.sup.2+]-dependent proteases; proteolysis

Published
2006

16. Effect of creatine on contractile force and sensitivity in mechanically skinned single fibers from rat skeletal muscle

Author

Murphy, Robyn M., Stephenson, D. George, and Lamb, Graham D.

Subjects
Fatigue -- Research, Creatine -- Research, Biological sciences
Abstract

Increasing the intramuscular stores of total creatine [TCr = creatine (Cr) + creatine phosphate (CrP)] can result in improved muscle performance during certain types of exercise in humans. Initial uptake of Cr is accompanied by an increase in cellular water to maintain osmotic balance, resulting in a decrease in myoplasmic ionic strength. Mechanically skinned single fibers from rat soleus (SOL) and extensor digitorum longus (EDL) muscles were used to examine the direct effects on the contractile apparatus of increasing [Cr], increasing [Cr] plus decreasing ionic strength, and increasing [Cr] and [CrP] with no change in ionic strength. Increasing [Cr] from 19 to 32 mM, accompanied by appropriate increases in water to maintain osmolality, had appreciable beneficial effects on contractile apparatus performance. Compared with control conditions, both SOL and EDL fibers showed increases in [Ca.sup.2+] sensitivity (+0.061 [+ or -] 0.004 and +0.049 [+ or -] 0.009 pCa units, respectively) and maximum [Ca.sup.2+]-activated force (to 104 [+ or -] 1 and 105 [+ or -] 1%, respectively). In contrast, increasing [Cr] alone had a small inhibitory effect. When both [Cr] and [CrP] were increased, there was virtually no change in [Ca.sup.2+] sensitivity of the contractile apparatus, and maximum [Ca.sup.2+]-activated force was ~106 [+ or -] 1% compared with control conditions in both SOL and EDL fibers. These results suggest that the initial improvement in performance observed with Cr supplementation is likely due in large part to direct effects of the accompanying decrease in myoplasmic ionic strength on the properties of the contractile apparatus. ergogenic aid; muscle contraction; fatigue

Published
2004

19. S-nitrosylation andS-glutathionylation of Cys134 on troponin I have opposing competitive actions on Ca2+sensitivity in rat fast-twitch muscle fibers

Author

G. S. Posterino, Janelle P. Mollica, Graham D. Lamb, Cedric R. Lamboley, David W. Greening, Travis L. Dutka, Robyn M. Murphy, and VC Weerakkody

Subjects
0301 basic medicine, Muscle fatigue, Physiology, Skeletal muscle, Cell Biology, Isometric exercise, S-Nitrosylation, Nitric oxide, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, chemistry, Biochemistry, Troponin I, Biophysics, medicine, S-Glutathionylation, 030217 neurology & neurosurgery, Peroxynitrite
Abstract

Nitric oxide is generated in skeletal muscle with activity and decreases Ca2+sensitivity of the contractile apparatus, putatively by S-nitrosylation of an unidentified protein. We investigated the mechanistic basis of this effect and its relationship to the oxidation-induced increase in Ca2+sensitivity in mammalian fast-twitch (FT) fibers mediated by S-glutathionylation of Cys134 on fast troponin I (TnIf). Force-[Ca2+] characteristics of the contractile apparatus in mechanically skinned fibers were assessed by direct activation with heavily Ca2+-buffered solutions. Treatment with S-nitrosylating agents, S-nitrosoglutathione (GSNO) or S-nitroso- N-acetyl-penicillamine (SNAP), decreased pCa50( = −log10[Ca2+] at half-maximal activation) by ~−0.07 pCa units in rat and human FT fibers without affecting maximum force, but had no effect on rat and human slow-twitch fibers or toad or chicken FT fibers, which all lack Cys134. The Ca2+sensitivity decrease was 1) fully reversed with dithiothreitol or reduced glutathione, 2) at least partially reversed with ascorbate, indicative of involvement of S-nitrosylation, and 3) irreversibly blocked by low concentration of the alkylating agent, N-ethylmaleimide (NEM). The biotin-switch assay showed that both GSNO and SNAP treatments caused S-nitrosylation of TnIf. S-glutathionylation pretreatment blocked the effects of S-nitrosylation on Ca2+sensitivity, and vice-versa. S-nitrosylation pretreatment prevented NEM from irreversibly blocking S-glutathionylation of TnIfand its effects on Ca2+sensitivity, and likewise S-glutathionylation pretreatment prevented NEM block of S-nitrosylation. Following substitution of TnIfinto rat slow-twitch fibers, S-nitrosylation treatment caused decreased Ca2+sensitivity. These findings demonstrate that S-nitrosylation and S-glutathionylation exert opposing effects on Ca2+sensitivity in mammalian FT muscle fibers, mediated by competitive actions on Cys134 of TnIf.

Published
2017

20. Perilipin 5 is dispensable for normal substrate metabolism and in the adaptation of skeletal muscle to exercise training

Author

Ruzaidi A. M. Mohktar, Robyn M. Murphy, Magdalene K. Montgomery, and Matthew J. Watt

Subjects
Male, 0301 basic medicine, medicine.medical_specialty, Time Factors, Physiology, Endocrinology, Diabetes and Metabolism, Muscle Proteins, Biology, Running, Mice, 03 medical and health sciences, Oxygen Consumption, Endurance training, Physical Conditioning, Animal, Physiology (medical), Internal medicine, Lipid droplet, medicine, Animals, Citrate synthase, Exercise physiology, Muscle, Skeletal, Triglycerides, Mice, Knockout, Exercise Tolerance, Organelle Biogenesis, Fatty Acids, Intracellular Signaling Peptides and Proteins, Skeletal muscle, Lipid metabolism, Lipid Metabolism, Adaptation, Physiological, Mitochondria, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Mitochondrial biogenesis, Perilipin, biology.protein, Carbohydrate Metabolism, Glycogen
Abstract

Cytoplasmic lipid droplets provide a reservoir for triglyceride storage and are a central hub for fatty acid trafficking in cells. The protein perilipin 5 (PLIN5) is highly expressed in oxidative tissues such as skeletal muscle and regulates lipid metabolism by coordinating the trafficking and the reversible interactions of effector proteins at the lipid droplet. PLIN5 may also regulate mitochondrial function, although this remains unsubstantiated. Hence, the aims of this study were to examine the role of PLIN5 in the regulation of skeletal muscle substrate metabolism during acute exercise and to determine whether PLIN5 is required for the metabolic adaptations and enhancement in exercise tolerance following endurance exercise training. Using muscle-specific Plin5 knockout mice ( Plin5MKO), we show that PLIN5 is dispensable for normal substrate metabolism during exercise, as reflected by levels of blood metabolites and rates of glycogen and triglyceride depletion that were indistinguishable from control (lox/lox) mice. Plin5MKOmice exhibited a functional impairment in their response to endurance exercise training, as reflected by reduced maximal running capacity (20%) and reduced time to fatigue during prolonged submaximal exercise (15%). The reduction in exercise performance was not accompanied by alterations in carbohydrate and fatty acid metabolism during submaximal exercise. Similarly, mitochondrial capacity (mtDNA, respiratory complex proteins, citrate synthase activity) and mitochondrial function (oxygen consumption rate in muscle fiber bundles) were not different between lox/lox and Plin5MKOmice. Thus, PLIN5 is dispensable for normal substrate metabolism during exercise and is not required to promote mitochondrial biogenesis or enhance the cellular adaptations to endurance exercise training.

Published
2016

21. When phosphorylated at Thr148, the β2-subunit of AMP-activated kinase does not associate with glycogen in skeletal muscle

Author

Noni T. Frankenberg, Robyn M. Murphy, Graham D. Lamb, Hongyang Xu, Paul R. Gooley, and David Stapleton

Subjects
Male, Threonine, 0301 basic medicine, medicine.medical_specialty, Time Factors, Physiology, Stimulation, AMP-Activated Protein Kinases, In Vitro Techniques, 5'-AMP-Activated Protein Kinase, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, AMP-activated protein kinase, Internal medicine, medicine, Animals, Phosphorylation, Protein kinase A, 030102 biochemistry & molecular biology, biology, Glycogen, AMPK, Skeletal muscle, Cell Biology, Electric Stimulation, Protein Subunits, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, chemistry, Biochemistry, Muscle Fibers, Fast-Twitch, biology.protein, medicine.symptom, Energy Metabolism, Acetyl-CoA Carboxylase, Muscle Contraction, Protein Binding, Muscle contraction
Abstract

The 5′-AMP-activated protein kinase (AMPK), a heterotrimeric complex that functions as an intracellular fuel sensor that affects metabolism, is activated in skeletal muscle in response to exercise and utilization of stored energy. The diffusibility properties of α- and β-AMPK were examined in isolated skeletal muscle fiber segments dissected from rat fast-twitch extensor digitorum longus and oxidative soleus muscles from which the surface membranes were removed by mechanical dissection. After the muscle segments were washed for 1 and 10 min, ∼60% and 75%, respectively, of the total AMPK pools were found in the diffusible fraction. After in vitro stimulation of the muscle, which resulted in an ∼80% decline in maximal force, 20% of the diffusible pool became bound in the fiber. This bound pool was not associated with glycogen, as determined by addition of a wash step containing amylase. Stimulation of extensor digitorum longus muscles resulted in 28% glycogen utilization and a 40% increase in phosphorylation of the downstream AMPK target acetyl carboxylase-CoA. This, however, had no effect on the proportion of total β2-AMPK that was phosphorylated in whole muscle homogenates measured by immunoprecipitation. These findings suggest that, in rat skeletal muscle, β2-AMPK is not associated with glycogen and that activation of AMPK by muscle contraction does not dephosphorylate β2-AMPK. These findings question the physiological relevance of the carbohydrate-binding function of β2-AMPK in skeletal muscle.

Published
2016

23. Glucose uptake during contraction in isolated skeletal muscles from neuronal nitric oxide synthase μ knockout mice

Author

Robyn M. Murphy, Glenn K. McConell, Gordon S. Lynch, Yet Hoi Hong, Tony Frugier, Xinmei Zhang, Stephen Rattigan, and Andrew C. Betik

Subjects
Male, medicine.medical_specialty, Contraction (grammar), Physiology, Glucose uptake, Nitric Oxide Synthase Type I, AMP-Activated Protein Kinases, Arginine, Nitric Oxide, Mice, Insulin resistance, AMP-activated protein kinase, Physical Conditioning, Animal, Physiology (medical), Internal medicine, medicine, Animals, Enzyme Inhibitors, Muscle, Skeletal, Mice, Knockout, omega-N-Methylarginine, biology, business.industry, Skeletal muscle, Biological Transport, medicine.disease, Mice, Inbred C57BL, Nitric oxide synthase, Glucose, Endocrinology, medicine.anatomical_structure, biology.protein, Omega-N-Methylarginine, Female, medicine.symptom, business, Muscle Contraction, Muscle contraction
Abstract

Inhibition of nitric oxide synthase (NOS) significantly attenuates the increase in skeletal muscle glucose uptake during contraction/exercise, and a greater attenuation is observed in individuals with Type 2 diabetes compared with healthy individuals. Therefore, NO appears to play an important role in mediating muscle glucose uptake during contraction. In this study, we investigated the involvement of neuronal NOSμ (nNOSμ), the main NOS isoform activated during contraction, on skeletal muscle glucose uptake during ex vivo contraction. Extensor digitorum longus muscles were isolated from nNOSμ−/−and nNOSμ+/+mice. Muscles were contracted ex vivo in a temperature-controlled (30°C) organ bath with or without the presence of the NOS inhibitor NG-monomethyl-l-arginine (L-NMMA) and the NOS substrate L-arginine. Glucose uptake was determined by radioactive tracers. Skeletal muscle glucose uptake increased approximately fourfold during contraction in muscles from both nNOSμ−/−and nNOSμ+/+mice. L-NMMA significantly attenuated the increase in muscle glucose uptake during contraction in both genotypes. This attenuation was reversed by L-arginine, suggesting that L-NMMA attenuated the increase in muscle glucose uptake during contraction by inhibiting NOS and not via a nonspecific effect of the inhibitor. Low levels of NOS activity (∼4%) were detected in muscles from nNOSμ−/−mice, and there was no evidence of compensation from other NOS isoform or AMP-activated protein kinase which is also involved in mediating muscle glucose uptake during contraction. These results indicate that NO regulates skeletal muscle glucose uptake during ex vivo contraction independently of nNOSμ.

Published
2015

24. Characterization of muscle ankyrin repeat proteins in human skeletal muscle

Author

Robyn M. Murphy, Stefan G. Wette, Heather K. Smith, and Graham D. Lamb

Subjects
0301 basic medicine, Physiology, Quantitative proteomics, Cardiac muscle, Skeletal muscle, Repressor, Cell Biology, Biology, Molecular biology, Rats sprague dawley, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, biology.protein, medicine, Titin, Ankyrin repeat, Nuclear protein, 030217 neurology & neurosurgery, Research Article
Abstract

Muscle ankyrin repeat proteins (MARPs) are a family of titin-associated, stress-response molecules and putative transducers of stretch-induced signaling in skeletal muscle. In cardiac muscle, cardiac ankyrin repeat protein (CARP) and diabetes-related ankyrin repeat protein (DARP) reportedly redistribute from binding sites on titin to the nucleus following a prolonged stretch. However, it is unclear whether ankyrin repeat domain protein 2 (Ankrd 2) shows comparable stretch-induced redistribution to the nucleus. We measured the following in rested human skeletal muscle: 1) the absolute amount of MARPs and 2) the distribution of Ankrd 2 and DARP in both single fibers and whole muscle preparations. In absolute amounts, Ankrd 2 is the most abundant MARP in human skeletal muscle, there being ~3.1 µmol/kg, much greater than DARP and CARP (~0.11 and ~0.02 µmol/kg, respectively). All DARP was found to be tightly bound at cytoskeletal (or possibly nuclear) sites. In contrast, ~70% of the total Ankrd 2 is freely diffusible in the cytosol [including virtually all of the phosphorylated (p)Ankrd 2-Ser99 form], ~15% is bound to non-nuclear membranes, and ~15% is bound at cytoskeletal sites, likely at the N2A region of titin. These data are not consistent with the proposal that Ankrd 2, per se, or pAnkrd 2-Ser99 mediates stretch-induced signaling in skeletal muscle, dissociating from titin and translocating to the nucleus, because the majority of these forms of Ankrd 2 are already free in the cytosol. It will be necessary to show that the titin-associated Ankrd 2 is modified by stretch in some as-yet-unidentified way, distinct from the diffusible pool, if it is to act as a stretch-sensitive signaling molecule.

Published
2017

25. Acute effects of taurine on sarcoplasmic reticulum Ca2+ accumulation and contractility in human type I and type II skeletal muscle fibers

Author

Cedric R. Lamboley, Graham D. Lamb, Travis L. Dutka, and Robyn M. Murphy

Subjects
Adult, Male, Acute effects, Taurine, medicine.medical_specialty, Adolescent, Physiology, Muscle Fibers, Skeletal, Single fiber, Skeletal Muscle Fibers, Human type, Biology, Contractile apparatus, Contractility, Young Adult, chemistry.chemical_compound, Physiology (medical), Internal medicine, medicine, Humans, Carnosine, Endoplasmic reticulum, Sarcoplasmic Reticulum, Endocrinology, chemistry, Biochemistry, Calcium, Female, Muscle Contraction
Abstract

Taurine occurs in high concentrations in muscle and is implicated in numerous physiological processes, yet its effects on many aspects of contractility remain unclear. Using mechanically skinned segments of human vastus lateralis muscle fibers, we characterized the effects of taurine on sarcoplasmic reticulum (SR) Ca2+ accumulation and contractile apparatus properties in type I and type II fibers. Prolonged myoplasmic exposure (>10 min) to taurine substantially increased the rate of accumulation of Ca2+ by the SR in both fiber types, with no change in the maximum amount accumulated; no such effect was found with carnosine. SR Ca2+ accumulation was similar with 10 or 20 mM taurine, but was significantly slower at 5 mM taurine. Cytoplasmic taurine (20 mM) had no detectable effects on the responsiveness of the Ca2+ release channels in either fiber type. Taurine caused a small increase in Ca2+ sensitivity of the contractile apparatus in type I fibers, but type II fibers were unaffected; maximum Ca2+-activated force was unchanged in both cases. The effects of taurine on SR Ca2+ accumulation 1) only became apparent after prolonged cytoplasmic exposure, and 2) persisted for some minutes after complete removal of taurine from the cytoplasm, consistent with the hypothesis that the effects were due to an action of taurine from inside the SR. In summary, taurine potentiates the rate of SR Ca2+ uptake in both type I and type II human fibers, possibly via an action from within the SR lumen, with the degree of potentiation being significantly reduced at low physiological taurine levels.

Published
2014

26. Elevated MMP2 abundance and activity in mdx mice are alleviated by prenatal taurine supplementation.

Author

Xiaoyu Ren, Hongyang Xu, Barker, Robert G., Lamb, Graham D., and Murphy, Robyn M.

Subjects
SKELETAL muscle, DUCHENNE muscular dystrophy, MICE, MUSCLE strength, MUSCLE growth, MUSCLE cells
Abstract

Elevated MMP2 abundance and activity in mdx mice are alleviated by prenatal taurine supplementation. Am J Physiol Cell Physiol 318: C1083-C1091, 2020. First published March 25, 2020; doi:10.1152/ajpcell.00437. 2019.--Duchenne muscular dystrophy (DMD) is a severe, progressive muscle-wasting disorder that leads to early death. The mdx mouse is a naturally occurring mutant model for DMD. It lacks dystrophin and displays peak muscle cell necrosis at ~28 days (D28), but in contrast to DMD, mdx mice experience muscle regeneration by D70. We hypothesized that matrix metalloproteinase-2 (MMP2) and/or MMP9 play key roles in the degeneration/regeneration phases in mdx mice. MMP2 abundance in muscle homogenates, measured by calibrated Western blotting, and activity, measured by zymogram, were lower at D70 compared with D28 in both mdx and wild-type (WT) mice. Importantly, MMP2 abundance was higher in both D28 and D70 mdx mice than in age-matched WT mice. The higher MMP2 abundance was not due to infiltrating macrophages, because MMP2 content was still higher in isolated muscle fibers where most macrophages had been removed. Prenatal supplementation with the amino acid taurine, which improved muscle strength in D28 mdx mice, produced approximately twofold lower MMP2 activity, indicating that increased MMP2 abundance is not required when muscle damage is attenuated. There was no difference in MMP9 abundance between age-matched WT and mdx mice (P > 0.05). WT mice displayed decreased MMP9 abundance as they aged. While MMP9 may have a role during age-related skeletal muscle growth, it does not appear essential for degeneration/regeneration cycles in the mdx mouse. Our findings indicate that MMP2 plays a more active role than MMP9 in the degenerative phases of muscle fibers in D28 mdx mice. [ABSTRACT FROM AUTHOR]

Published
2020
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30. Influences of temperature, oxidative stress, and phosphorylation on binding of heat shock proteins in skeletal muscle fibers

Author

Noni T. Larkins, Robyn M. Murphy, and Graham D. Lamb

Subjects
Male, Hot Temperature, Physiology, Chemistry, Muscle Fibers, Skeletal, Temperature, HSP72 Heat-Shock Proteins, Skeletal Muscle Fibers, Cell Biology, medicine.disease_cause, Rats, Cell biology, Fight-or-flight response, Oxidative Stress, Organ Culture Techniques, Biochemistry, Heat shock protein, medicine, Animals, Phosphorylation, Rats, Long-Evans, Function (biology), Oxidative stress, Protein Binding
Abstract

Heat shock proteins (HSPs) help maintain cellular function in stressful situations, but the processes controlling their interactions with target proteins are not well defined. This study examined the binding of HSP72, HSP25, and αB-crystallin in skeletal muscle fibers following various stresses. Rat soleus (SOL) and extensor digitorum longus (EDL) muscles were subjected in vitro to heat stress or strongly fatiguing stimulation. Superficial fibers were “skinned” by microdissection and HSP diffusibility assessed from the extent of washout following 10- to 30 min exposure to a physiological intracellular solution. In fibers from nonstressed (control) SOL muscle, >80% of each HSP is readily diffusible. However, after heating a muscle to 40°C for 30 min ∼95% of HSP25 and αB-crystallin becomes tightly bound at nonmembranous myofibrillar sites, whereas HSP72 bound at membranous sites only after heat treatment to ≥44°C. The ratio of reduced to oxidized cytoplasmic glutathione (GSH:GSSG) decreased approximately two- and fourfold after heating muscles to 40° and 45°C, respectively. The reducing agent dithiothreitol reversed HSP72 binding in heated muscles but had no effect on the other HSPs. Intense in vitro stimulation of SOL muscles, sufficient to elicit substantial oxidation-related loss of maximum force and approximately fourfold decrease in the GSH:GSSG ratio, had no effect on diffusibility of any of the HSPs. When skinned fibers from heat-treated muscles were bathed with additional exogenous HSP72, total binding increased approximately two- and 10-fold, respectively, in SOL and EDL fibers, possibly reflective of the relative sarco(endo)plasmic reticulum Ca2+-ATPase pump densities in the two fiber types. Phosphorylation at Ser59 on αB-crystallin and Ser85 on HSP25 increased with heat treatment but did not appear to determine HSP binding. The findings highlight major differences in the processes controlling binding of HSP72 and the two small HSPs. Binding was not directly related to cytoplasmic oxidative status, but oxidation of cysteine residues influenced HSP72 binding.

Published
2012

31. Effects of carnosine on contractile apparatus Ca2+sensitivity and sarcoplasmic reticulum Ca2+release in human skeletal muscle fibers

Author

Travis L. Dutka, Robyn M. Murphy, Cedric R. Lamboley, Graham D. Lamb, and Michael J. McKenna

Subjects
Calcium metabolism, Physiology, Ryanodine receptor, Chemistry, Endoplasmic reticulum, Skeletal muscle, Carnosine, Anatomy, Contractile apparatus, Coupling (electronics), chemistry.chemical_compound, medicine.anatomical_structure, Physiology (medical), medicine, Biophysics, Calcium-induced calcium release
Abstract

There is considerable interest in potential ergogenic and therapeutic effects of increasing skeletal muscle carnosine content, although its effects on excitation-contraction (EC) coupling in human muscle have not been defined. Consequently, we sought to characterize what effects carnosine, at levels attained by supplementation, has on human muscle fiber function, using a preparation with all key EC coupling proteins in their in situ positions. Fiber segments, obtained from vastus lateralis muscle of human subjects by needle biopsy, were mechanically skinned, and their Ca2+release and contractile apparatus properties were characterized. Ca2+sensitivity of the contractile apparatus was significantly increased by 8 and 16 mM carnosine (increase in pCa50of 0.073 ± 0.007 and 0.116 ± 0.006 pCa units, respectively, in six type I fibers, and 0.063 ± 0.018 and 0.103 ± 0.013 pCa units, respectively, in five type II fibers). Caffeine-induced force responses were potentiated by 8 mM carnosine in both type I and II fibers, with the potentiation in type II fibers being entirely explicable by the increase in Ca2+sensitivity of the contractile apparatus caused by carnosine. However, the potentiation of caffeine-induced responses caused by carnosine in type I fibers was beyond that expected from the associated increase in Ca2+sensitivity of the contractile apparatus and suggestive of increased Ca2+-induced Ca2+release. Thus increasing muscle carnosine content likely confers benefits to muscle performance in both fiber types by increasing the Ca2+sensitivity of the contractile apparatus and possibly also by aiding Ca2+release in type I fibers, helping to lessen or slow the decline in muscle performance during fatiguing stimulation.

Published
2012

32. Reply to 'Letter to the editor: Comments on Wette et al. (2017): ‘Characterization of muscle ankyrin repeat proteins in human skeletal muscle’'

Author

Stefan G. Wette, Robyn M. Murphy, Heather K. Smith, and Graham D. Lamb

Subjects
0301 basic medicine, Gerontology, Letter to the editor, Physiology, business.industry, Muscle Proteins, Skeletal muscle, Cell Biology, Characterization (mathematics), Ankyrin Repeat, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Humans, Medicine, Ankyrin repeat, Muscle, Skeletal, business, Neuroscience
Abstract

we appreciate the interest in our recently published study ([6][1]) shown by the Letter to the editor by Dr. Cenni ([2][2]), but we are compelled to point out that the main criticisms made are entirely misplaced and that the Letter includes some major misstatements about findings in the literature

Published
2017

33. Quantification of calsequestrin 2 (CSQ2) in sheep cardiac muscle and Ca2+-binding protein changes in CSQ2 knockout mice

Author

Graham D. Lamb, Robyn M. Murphy, Nicole A. Beard, Janelle P. Mollica, and Bjorn C. Knollmann

Subjects
Silver Staining, medicine.medical_specialty, Physiology, Heart Ventricles, Blotting, Western, Calcium buffering, chemistry.chemical_element, Calcium, Calsequestrin, Mice, Physiology (medical), Calcium-binding protein, Internal medicine, medicine, Animals, Calcium signaling, Mice, Knockout, Sheep, Cardiac Excitation and Contraction, Myocardium, Spectrophotometry, Atomic, Endoplasmic reticulum, Calcium-Binding Proteins, Cardiac muscle, Rats, Cell biology, Sarcoplasmic Reticulum, medicine.anatomical_structure, Endocrinology, chemistry, Knockout mouse, Cardiology and Cardiovascular Medicine
Abstract

Calsequestrin 2 (CSQ2) is generally regarded as the primary Ca2+-buffering molecule present inside the sarcoplasmic reticulum (SR) in cardiac cells, but findings from CSQ2 knockout experiments raise major questions about its role and necessity. This study determined the absolute amount of CSQ2 present in cardiac ventricular muscle to gauge its likely influence on SR free Ca2+concentration ([Ca2+]) and maximal Ca2+capacity. Ventricular tissue from hearts of freshly killed sheep was examined by SDS-PAGE without any fractionation, and CSQ2 was detected by Western blotting; this method avoided the >90% loss of CSQ2 occurring with usual fractionation procedures. Band intensities were compared against those for purified CSQ2 run on the same blots. Fidelity of quantification was verified by demonstrating that CSQ2 added to homogenates was detected with equal efficacy as purified CSQ2 alone. Ventricular tissue from sheep ( n = 8) contained 24 ± 2 μmol CSQ2/kg wet wt. Total Ca2+content of the ventricular tissue, measured by atomic absorption spectroscopy, was 430 ± 20 μmol/kg (with SR Ca2+likely 2+per CSQ2. The large amount of CSQ2 bestows the SR with a high theoretical maximal Ca2+-binding capacity (∼1 mmol Ca2+/kg ventricular tissue, assuming a maximum of ∼40 Ca2+per CSQ2) and would keep free [Ca2+] within the SR relatively low, energetically favoring Ca2+uptake and reducing SR leak. In mice with CSQ2 ablated, histidine-rich Ca2+-binding protein was upregulated ∼35% in ventricular tissue, possibly in compensation.

Published
2011

34. Upregulation of store-operated Ca2+ entry in dystrophic mdx mouse muscle

Author

Robyn M. Murphy, Frederic von Wegner, Tanya R. Cully, Joshua N. Edwards, Oliver Friedrich, and Bradley S. Launikonis

Subjects
Cytoplasm, medicine.medical_specialty, mdx mouse, ORAI1 Protein, Physiology, Ratón, In Vitro Techniques, Biology, Muscular Dystrophies, Mice, Downregulation and upregulation, Internal medicine, medicine, Animals, Calcium Signaling, Stromal Interaction Molecule 1, Muscular dystrophy, Muscle, Skeletal, Excitation Contraction Coupling, Membrane Glycoproteins, Microscopy, Confocal, ORAI1, Endoplasmic reticulum, Skeletal muscle, STIM1, Cell Biology, medicine.disease, Disease Models, Animal, Kinetics, Sarcoplasmic Reticulum, medicine.anatomical_structure, Endocrinology, Mice, Inbred mdx, Calcium Channels, Ion Channel Gating
Abstract

Store-operated Ca2+ entry (SOCE) is an important mechanism in virtually all cells. In adult skeletal muscle, this mechanism is highly specialized for the rapid delivery of Ca2+ from the transverse tubule into the junctional cleft during periods of depleting Ca2+ release. In dystrophic muscle fibers, SOCE may be a source of Ca2+ overload, leading to cell necrosis. However, this possibility is yet to be examined in an adult fiber during Ca2+ release. To examine this, Ca2+ in the tubular system and cytoplasm were simultaneously imaged during direct release of Ca2+ from sarcoplasmic reticulum (SR) in skeletal muscle fibers from healthy (wild-type, WT) and dystrophic mdx mouse. The mdx fibers were found to have normal activation and deactivation properties of SOCE. However, a depression of the cytoplasmic Ca2+ transient in mdx compared with WT fibers was observed, as was a shift in the SOCE activation and deactivation thresholds to higher SR Ca2+ concentrations ([Ca2+]SR). The shift in SOCE activation and deactivation thresholds was accompanied by an approximately threefold increase in STIM1 and Orai1 proteins in dystrophic muscle. While the mdx fibers can introduce more Ca2+ into the fiber for an equivalent depletion of [Ca2+]SR via SOCE, it remains unclear whether this is deleterious.

Published
2010

35. Taurine supplementation increases skeletal muscle force production and protects muscle function during and after high-frequency in vitro stimulation

Author

Christos G. Stathis, Kevin D. Croft, Trevor A. Mori, Robyn M. Murphy, Craig A. Goodman, Deanna Horvath, and Alan Hayes

Subjects
Male, medicine.medical_specialty, Taurine, Physiology, Endogeny, Stimulation, In Vitro Techniques, Rats, Sprague-Dawley, Contractility, chemistry.chemical_compound, Water Supply, Physiology (medical), Internal medicine, medicine, Animals, Calsequestrin, Muscle, Skeletal, Membrane Glycoproteins, biology, Muscle fatigue, Calcium-Binding Proteins, Membrane Transport Proteins, Skeletal muscle, Calpain, Articles, Electric Stimulation, Rats, Endocrinology, medicine.anatomical_structure, chemistry, Biochemistry, Muscle Fatigue, Muscle Fibers, Fast-Twitch, biology.protein, medicine.symptom, Carrier Proteins, Muscle Contraction, Muscle contraction
Abstract

Recent studies report that depletion and repletion of muscle taurine (Tau) to endogenous levels affects skeletal muscle contractility in vitro. In this study, muscle Tau content was raised above endogenous levels by supplementing male Sprague-Dawley rats with 2.5% (wt/vol) Tau in drinking water for 2 wk, after which extensor digitorum longus (EDL) muscles were examined for in vitro contractile properties, fatigue resistance, and recovery from fatigue after two different high-frequency stimulation bouts. Tau supplementation increased muscle Tau content by ∼40% and isometric twitch force by 19%, shifted the force-frequency relationship upward and to the left, increased specific force by 4.2%, and increased muscle calsequestrin protein content by 49%. Force at the end of a 10-s (100 Hz) continuous tetanic stimulation was 6% greater than controls, while force at the end of the 3-min intermittent high-frequency stimulation bout was significantly higher than controls, with a 12% greater area under the force curve. For 1 h after the 10-s continuous stimulation, tetanic force in Tau-supplemented muscles remained relatively stable while control muscle force gradually deteriorated. After the 3-min intermittent bout, tetanic force continued to slowly recover over the next 1 h, while control muscle force again began to decline. Tau supplementation attenuated F2-isoprostane production (a sensitive indicator of reactive oxygen species-induced lipid peroxidation) during the 3-min intermittent stimulation bout. Finally, Tau transporter protein expression was not altered by the Tau supplementation. Our results demonstrate that raising Tau content above endogenous levels increases twitch and subtetanic and specific force in rat fast-twitch skeletal muscle. Also, we demonstrate that raising Tau protects muscle function during high-frequency in vitro stimulation and the ensuing recovery period and helps reduce oxidative stress during prolonged stimulation.

Published
2009

38. Inflammation and lung injury in an ovine model of extracorporeal membrane oxygenation support

Author

Passmore, Margaret R., primary, Fung, Yoke L., additional, Simonova, Gabriela, additional, Foley, Samuel R., additional, Dunster, Kimble R., additional, Diab, Sara D., additional, Tung, John-Paul, additional, Minchinton, Robyn M., additional, McDonald, Charles I., additional, Anstey, Chris M., additional, Shekar, Kiran, additional, and Fraser, John F., additional

Published
2016
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42. Cold-water immersion after training sessions: effects on fiber type-specific adaptations in muscle K + transport proteins to sprint-interval training in men.

Author

Christiansen, Danny, Bishop, David J., Broatch, James R., Bangsbo, Jens, McKenna, Michael J., and Murphy, Robyn M.

Abstract

Effects of regular use of cold-water immersion (CWI) on fiber type-specific adaptations in muscle K+ transport proteins to intense training, along with their relationship to changes in mRNA levels after the first training session, were investigated in humans. Nineteen recreationally active men (24 ± 6 yr, 79.5 ± 10.8 kg, 44.6 ± 5.8 ml·kg-1·min-1) completed six weeks of sprint-interval cycling, either without (passive rest; CON) or with training sessions followed by CWI (15 min at 10°C; COLD). Muscle biopsies were obtained before and after training to determine abundance of Na+, K+-ATPase isoforms (α1-3, β1-3) and phospholemman (FXYD1) and after recovery treatments (+0 h and +3 h) on the first day of training to measure mRNA content. Training increased ( P < 0.05) the abundance of α1 and β3 in both fiber types and β1 in type-II fibers and decreased FXYD1 in type-I fibers, whereas α2 and α3 abundance was not altered by training ( P > 0.05). CWI after each session did not influence responses to training ( P > 0.05). However, α2 mRNA increased after the first session in COLD (+0 h, P < 0.05) but not in CON ( P > 0.05). In both conditions, α1 and β3 mRNA increased (+3 h; P < 0.05) and β2 mRNA decreased (+3 h; P < 0.05), whereas α3, β1, and FXYD1 mRNA remained unchanged ( P > 0.05) after the first session. In summary, Na+,K+-ATPase isoforms are differently regulated in type I and II muscle fibers by sprint-interval training in humans, which, for most isoforms, do not associate with changes in mRNA levels after the first training session. CWI neither impairs nor improves protein adaptations to intense training of importance for muscle K+ regulation. NEW & NOTEWORTHY Although cold-water immersion (CWI) after training and competition has become a routine for many athletes, limited published evidence exists regarding its impact on training adaptation. Here, we show that CWI can be performed regularly without impairing training-induced adaptations at the fiber-type level important for muscle K+ handling. Furthermore, sprint-interval training invoked fiber type-specific adaptations in K+ transport proteins, which may explain the dissociated responses of whole-muscle protein levels and K+ transport function to training previously reported. [ABSTRACT FROM AUTHOR]

Published
2018
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46. Dissociation between short-term unloading and resistance training effects on skeletal muscle Na+,K+-ATPase, muscle function, and fatigue in humans.

Author

Perry, Ben D., Wyckelsma, Victoria L., Murphy, Robyn M., Steward, Collene H., Anderson, Mitchell, Levinger, Itamar, Petersen, Aaron C., and McKenna, Michael J.

Subjects
SKELETAL muscle, ADENOSINE triphosphatase
Abstract

Physical training increases skeletal muscle Na+,K+-ATPase content (NKA) and improves exercise performance, but the effects of inactivity per se on NKA content and isoform abundance in human muscle are unknown. We investigated the effects of 23-day unilateral lower limb suspension (ULLS) and subsequent 4-wk resistance training (RT) on muscle function and NKA in 6 healthy adults, measuring quadriceps muscle peak torque; fatigue and venous [K+] during intense one-legged cycling exercise; and skeletal muscle NKA content ([³H]ouabain binding) and NKA isoform abundances (immunoblotting) in muscle homogenates (α1-3, β1-2) and in single fibers (α1-3, β1). In the unloaded leg after ULLS, quadriceps peak torque and cycling time to fatigue declined by 22 and 23%, respectively, which were restored with RT. Whole muscle NKA content and homogenate NKA α1-3 and β1-2 isoform abundances were unchanged with ULLS or RT. However, in single muscle fibers, NKA α3 in type I (-66%, P = 0.006) and β1 in type II fibers (-40%, P = 0.016) decreased after ULLS, with other NKA isoforms unchanged. After RT, NKA α1 (79%, P = 0.004) and β1 (35%, P = 0.01) increased in type II fibers, while α2 (76%, P = 0.028) and α3 (142%, P = 0.004) increased in type I fibers compared with post-ULLS. Despite considerably impaired muscle function and earlier fatigue onset, muscle NKA content and homogenate α1 and α2 abundances were unchanged, thus being resilient to inactivity induced by ULLS. Nonetheless, fiber type-specific downregulation with inactivity and upregulation with RT of several NKA isoforms indicate complex regulation of muscle NKA expression in humans. [ABSTRACT FROM AUTHOR]

Published
2016
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47. When phosphorylated at Thr148, the β2-subunit of AMP-activated kinase does not associate with glycogen in skeletal muscle.

Author

Hongyang Xu, Frankenberg, Noni T., Lamb, Graham D., Gooley, Paul R., Stapleton, David I., and Murphy, Robyn M.

Subjects
CYCLIC-AMP-dependent protein kinase, CARBOHYDRATES, BINDING agents, SKELETAL muscle, GLYCOGEN
Abstract

The 5'-AMP-activated protein kinase (AMPK), a heterotrimeric complex that functions as an intracellular fuel sensor that affects metabolism, is activated in skeletal muscle in response to exercise and utilization of stored energy. The diffusibility properties of α- and β-AMPK were examined in isolated skeletal muscle fiber segments dissected from rat fast-twitch extensor digitorum longus and oxidative soleus muscles from which the surface membranes were removed by mechanical dissection. After the muscle segments were washed for 1 and 10 min, 60% and 75%, respectively, of the total AMPK pools were found in the diffusible fraction. After in vitro stimulation of the muscle, which resulted in an80% decline in maximal force, 20% of the diffusible pool became bound in the fiber. This bound pool was not associated with glycogen, as determined by addition of a wash step containing amylase. Stimulation of extensor digitorum longus muscles resulted in 28% glycogen utilization and a 40% increase in phosphorylation of the downstream AMPK target acetyl carboxylase-CoA. This, however, had no effect on the proportion of total β2-AMPK that was phosphorylated in whole muscle homogenates measured by immuno-precipitation. These findings suggest that, in rat skeletal muscle, β2-AMPK is not associated with glycogen and that activation of AMPK by muscle contraction does not dephosphorylate β2-AMPK. These findings question the physiological relevance of the carbohydrate-binding function of β2-AMPK in skeletal muscle. [ABSTRACT FROM AUTHOR]

Published
2016
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