Increasing autophagy does not affect neurogenic muscle atrophy

Physiological autophagy plays a crucial role in the regulation of muscle mass and metabolism, while the excessive induction or the inhibition of the autophagic flux contributes to the progression of several diseases. Autophagy can be activated by different stimuli, including cancer, exercise, caloric restriction and denervation. The latter leads to muscle atrophy through the activation of catabolic pathways, i.e. the ubiquitin-proteasome system and autophagy. However, the kinetics of autophagy activation and the upstream molecular pathways in denervated skeletal muscle have not been reported yet. In this study, we characterized the kinetics of autophagic induction, quickly triggered by denervation, and report the Akt/mTOR axis activation. Besides, with the aim to assess the relative contribution of autophagy in neurogenic muscle atrophy, we triggered autophagy with different stimuli along with denervation, and observed that four week-long autophagic induction, by either intermitted fasting or rapamycin treatment, did not significantly affect muscle mass loss. We conclude that: i) autophagy does not play a major role in inducing muscle loss following denervation; ii) nonetheless, autophagy may have a regulatory role in denervation induced muscle atrophy, since it is significantly upregulated as early as eight hours after denervation; iii) Akt/mTOR axis, AMPK and FoxO3a are activated consistently with the progression of muscle atrophy, further highlighting the complexity of the signaling response to the atrophying stimulus deriving from denervation.

Download Full-text

Denervation does not induce muscle atrophy through oxidative stress

European Journal of Translational Myology ◽

10.4081/ejtm.2017.6406 ◽

2017 ◽

Vol 27 (1) ◽

Cited By ~ 8

Author(s):

Eva Pigna ◽

Emanuela Greco ◽

Giulio Morozzi ◽

Silvia Grottelli ◽

Alessio Rotini ◽

...

Keyword(s):

Oxidative Stress ◽

Skeletal Muscle ◽

Stress Response ◽

Muscle Atrophy ◽

Oxidative Stress Response ◽

Skeletal Muscle Atrophy ◽

Molecular Pathways ◽

Ubiquitin Proteasome ◽

Anti Oxidant ◽

Kinetics Of

Denervation leads to the activation of the catabolic pathways, such as the ubiquitin-proteasome and autophagy, resulting in skeletal muscle atrophy and weakness. Furthermore, denervation induces oxidative stress in skeletal muscle, which is thought to contribute to the induction of skeletal muscle atrophy. Several muscle diseases are characterized by denervation, but the molecular pathways contributing to muscle atrophy have been only partially described. Our study delineates the kinetics of activation of oxidative stress response in skeletal muscle following denervation. Despite the denervation-dependent induction of oxidative stress in skeletal muscle, treatments with anti-oxidant drugs do not prevent the reduction of muscle mass. Our results indicate that, although oxidative stress may contribute to the activation of the response to denervation, it is not responsible by itself of oxidative damage or neurogenic muscle atrophy.

Download Full-text

Involvement of AMPK in regulating slow-twitch muscle atrophy during hindlimb unloading in mice

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.00165.2015 ◽

2015 ◽

Vol 309 (7) ◽

pp. E651-E662 ◽

Cited By ~ 31

Author(s):

Tatsuro Egawa ◽

Ayumi Goto ◽

Yoshitaka Ohno ◽

Shingo Yokoyama ◽

Akihiro Ikuta ◽

...

Keyword(s):

Skeletal Muscle ◽

Protein Degradation ◽

Muscle Mass ◽

Muscle Atrophy ◽

Skeletal Muscle Mass ◽

Ubiquitin Proteasome System ◽

Hindlimb Unloading ◽

Slow Twitch Muscle ◽

Ubiquitin Proteasome ◽

Slow Twitch

AMPK is considered to have a role in regulating skeletal muscle mass. However, there are no studies investigating the function of AMPK in modulating skeletal muscle mass during atrophic conditions. In the present study, we investigated the difference in unloading-associated muscle atrophy and molecular functions in response to 2-wk hindlimb suspension between transgenic mice overexpressing the dominant-negative mutant of AMPK (AMPK-DN) and their wild-type (WT) littermates. Male WT ( n = 24) and AMPK-DN ( n = 24) mice were randomly divided into two groups: an untreated preexperimental control group ( n = 12 in each group) and an unloading ( n = 12 in each group) group. The relative soleus muscle weight and fiber cross-sectional area to body weight were decreased by ∼30% in WT mice by hindlimb unloading and by ∼20% in AMPK-DN mice. There were no changes in puromycin-labeled protein or Akt/70-kDa ribosomal S6 kinase signaling, the indicators of protein synthesis. The expressions of ubiquitinated proteins and muscle RING finger 1 mRNA and protein, markers of the ubiquitin-proteasome system, were increased by hindlimb unloading in WT mice but not in AMPK-DN mice. The expressions of molecules related to the protein degradation system, phosphorylated forkhead box class O3a, inhibitor of κBα, microRNA (miR)-1, and miR-23a, were decreased only in WT mice in response to hindlimb unloading, and 72-kDa heat shock protein expression was higher in AMPK-DN mice than in WT mice. These results imply that AMPK partially regulates unloading-induced atrophy of slow-twitch muscle possibly through modulation of the protein degradation system, especially the ubiquitin-proteasome system.

Download Full-text

Supplementation of ketoacids contributes to the up-regulation of the Wnt7a/Akt/p70S6K pathway and the down-regulation of apoptotic and ubiquitin–proteasome systems in the muscle of 5/6 nephrectomised rats

British Journal Of Nutrition ◽

10.1017/s0007114513004091 ◽

2014 ◽

Vol 111 (9) ◽

pp. 1536-1548 ◽

Cited By ~ 25

Author(s):

Dong-Tao Wang ◽

Lu Lu ◽

Ying Shi ◽

Zhen-Bo Geng ◽

Yi Yin ◽

...

Keyword(s):

Muscle Mass ◽

Muscle Atrophy ◽

Caspase 3 ◽

Ring Finger ◽

Ubiquitin Proteasome System ◽

Protein Diet ◽

Down Regulation ◽

Beneficial Effects ◽

Phosphorylated Akt ◽

Ubiquitin Proteasome

Ketoacids (KA) are known to improve muscle mass among patients with chronic kidney disease (CKD) on a low-protein diet (CKD-LPD), but the mechanism of its preventive effects on muscle atrophy still remains unclear. Since muscle atrophy in CKD may be attributable to the down-regulation of the Wnt7a/Akt/p70S6K pathway and the activation of the ubiquitin–proteasome system (UPS) and the apoptotic signalling pathway, a hypothesis can readily be drawn that KA supplementation improves muscle mass by up-regulating the Wnt7a/Akt/p70S6K pathway and counteracting the activation of the UPS and caspase-3-dependent apoptosis in the muscle of CKD-LPD rats. Rats with 5/6 nephrectomy were randomly divided into three groups, and fed with either 22 % protein (normal-protein diet; NPD), 6 % protein (LPD) or 5 % protein plus 1 % KA for 24 weeks. Sham-operated rats with NPD intake were used as the control. The results demonstrated that KA supplementation improved protein synthesis and increased related mediators such as Wnt7a, phosphorylated Akt and p70S6K in the muscle of CKD-LPD rats. It also inhibited protein degradation, withheld the increase in ubiquitin and its ligases MAFbx (muscle atrophy F-box) and MuRF1 (muscle ring finger-1) as well as attenuated proteasome activity in the muscle of CKD-LPD rats. Moreover, KA supplementation gave rise to a reduction in DNA fragment, cleaved caspase-3 and 14 kDa actin fragment via the down-regulation of the Bax:Bcl-2 ratio in the muscle of CKD-LPD rats. The beneficial effects unveiled herein further consolidate that KA may be a better therapeutic strategy for muscle atrophy in CKD-LPD.

Download Full-text

Identification of the MuRF1 skeletal muscle ubiquitylome through quantitative proteomics

Function ◽

10.1093/function/zqab029 ◽

2021 ◽

Author(s):

Leslie M Baehr ◽

David C Hughes ◽

Sarah A Lynch ◽

Delphi Van Haver ◽

Teresa Mendes Maia ◽

...

Keyword(s):

Skeletal Muscle ◽

Muscle Atrophy ◽

Potential Role ◽

Ubiquitin Proteasome System ◽

In Vivo Electroporation ◽

Adult Mice ◽

Expression Of Genes ◽

Regulation Of Metabolism ◽

Ubiquitin Proteasome

Abstract MuRF1 (TRIM63) is a muscle-specific E3 ubiquitin ligase and component of the ubiquitin proteasome system. MuRF1 is transcriptionally upregulated under conditions that cause muscle loss, in both rodents and humans, and is a recognized marker of muscle atrophy. In this study, we used in vivo electroporation to determine if MuRF1 overexpression alone can cause muscle atrophy and, in combination with ubiquitin proteomics, identify the endogenous MuRF1 substrates in skeletal muscle. Overexpression of MuRF1 in adult mice increases ubiquitination of myofibrillar and sarcoplasmic proteins, increases expression of genes associated with neuromuscular junction instability, and causes muscle atrophy. A total of 169 ubiquitination sites on 56 proteins were found to be regulated by MuRF1. MuRF1-mediated ubiquitination targeted both thick and thin filament contractile proteins, as well as, glycolytic enzymes, deubiquitinases, p62, and VCP. These data reveal a potential role for MuRF1 in not only the breakdown of the sarcomere, but also the regulation of metabolism and other proteolytic pathways in skeletal muscle.

Download Full-text

Activation of the ubiquitin-proteasome system contributes to oculopharyngeal muscular dystrophy through muscle atrophy

PLoS Genetics ◽

10.1371/journal.pgen.1010015 ◽

2022 ◽

Vol 18 (1) ◽

pp. e1010015

Author(s):

Cécile Ribot ◽

Cédric Soler ◽

Aymeric Chartier ◽

Sandy Al Hayek ◽

Rima Naït-Saïdi ◽

...

Keyword(s):

Muscular Dystrophy ◽

Muscle Atrophy ◽

Late Onset ◽

Oral Treatment ◽

Ubiquitin Proteasome System ◽

Proteasome Activity ◽

Functional Study ◽

Oculopharyngeal Muscular Dystrophy ◽

Ubiquitin Proteasome ◽

And Function

Oculopharyngeal muscular dystrophy (OPMD) is a late-onset disorder characterized by progressive weakness and degeneration of specific muscles. OPMD is due to extension of a polyalanine tract in poly(A) binding protein nuclear 1 (PABPN1). Aggregation of the mutant protein in muscle nuclei is a hallmark of the disease. Previous transcriptomic analyses revealed the consistent deregulation of the ubiquitin-proteasome system (UPS) in OPMD animal models and patients, suggesting a role of this deregulation in OPMD pathogenesis. Subsequent studies proposed that UPS contribution to OPMD involved PABPN1 aggregation. Here, we use a Drosophila model of OPMD to address the functional importance of UPS deregulation in OPMD. Through genome-wide and targeted genetic screens we identify a large number of UPS components that are involved in OPMD. Half dosage of UPS genes reduces OPMD muscle defects suggesting a pathological increase of UPS activity in the disease. Quantification of proteasome activity confirms stronger activity in OPMD muscles, associated with degradation of myofibrillar proteins. Importantly, improvement of muscle structure and function in the presence of UPS mutants does not correlate with the levels of PABPN1 aggregation, but is linked to decreased degradation of muscle proteins. Oral treatment with the proteasome inhibitor MG132 is beneficial to the OPMD Drosophila model, improving muscle function although PABPN1 aggregation is enhanced. This functional study reveals the importance of increased UPS activity that underlies muscle atrophy in OPMD. It also provides a proof-of-concept that inhibitors of proteasome activity might be an attractive pharmacological approach for OPMD.

Download Full-text

Exercise Mitigates the Loss of Muscle Mass by Attenuating the Activation of Autophagy during Severe Energy Deficit

Nutrients ◽

10.3390/nu11112824 ◽

2019 ◽

Vol 11 (11) ◽

pp. 2824 ◽

Cited By ~ 2

Author(s):

Marcos Martin-Rincon ◽

Alberto Pérez-López ◽

David Morales-Alamo ◽

Ismael Perez-Suarez ◽

Pedro de Pablos-Velasco ◽

...

Keyword(s):

Skeletal Muscle ◽

Muscle Mass ◽

Prolonged Exercise ◽

Control Diet ◽

Energy Deficit ◽

Muscle Loss ◽

Volume Changes ◽

Autophagy Induction ◽

Ubiquitin Proteasome ◽

Proteasome Pathway

The loss of skeletal muscle mass with energy deficit is thought to be due to protein breakdown by the autophagy-lysosome and the ubiquitin-proteasome systems. We studied the main signaling pathways through which exercise can attenuate the loss of muscle mass during severe energy deficit (5500 kcal/day). Overweight men followed four days of caloric restriction (3.2 kcal/kg body weight day) and prolonged exercise (45 min of one-arm cranking and 8 h walking/day), and three days of control diet and restricted exercise, with an intra-subject design including biopsies from muscles submitted to distinct exercise volumes. Gene expression and signaling data indicate that the main catabolic pathway activated during severe energy deficit in skeletal muscle is the autophagy-lysosome pathway, without apparent activation of the ubiquitin-proteasome pathway. Markers of autophagy induction and flux were reduced by exercise primarily in the muscle submitted to an exceptional exercise volume. Changes in signaling are associated with those in circulating cortisol, testosterone, cortisol/testosterone ratio, insulin, BCAA, and leucine. We conclude that exercise mitigates the loss of muscle mass by attenuating autophagy activation, blunting the phosphorylation of AMPK/ULK1/Beclin1, and leading to p62/SQSTM1 accumulation. This includes the possibility of inhibiting autophagy as a mechanism to counteract muscle loss in humans under severe energy deficit.

Download Full-text

Calpain and caspase-3 play required roles in immobilization-induced limb muscle atrophy

Journal of Applied Physiology ◽

10.1152/japplphysiol.00925.2012 ◽

2013 ◽

Vol 114 (10) ◽

pp. 1482-1489 ◽

Cited By ~ 50

Author(s):

Erin E. Talbert ◽

Ashley J. Smuder ◽

Kisuk Min ◽

Oh Sung Kwon ◽

Scott K. Powers

Keyword(s):

Muscle Atrophy ◽

Caspase 3 ◽

Respiratory Muscles ◽

Ubiquitin Proteasome System ◽

Type I ◽

Disuse Atrophy ◽

Limb Muscle ◽

Disuse Muscle Atrophy ◽

Ubiquitin Proteasome ◽

Rat Soleus Muscle

Prolonged skeletal muscle inactivity results in a rapid decrease in fiber size, primarily due to accelerated proteolysis. Although several proteases are known to contribute to disuse muscle atrophy, the ubiquitin proteasome system is often considered the most important proteolytic system during many conditions that promote muscle wasting. Emerging evidence suggests that calpain and caspase-3 may also play key roles in inactivity-induced atrophy of respiratory muscles, but it remains unknown if these proteases are essential for disuse atrophy in limb skeletal muscles. Therefore, we tested the hypothesis that activation of both calpain and caspase-3 is required for locomotor muscle atrophy induced by hindlimb immobilization. Seven days of immobilization (i.e., limb casting) promoted significant atrophy in type I muscle fibers of the rat soleus muscle. Independent pharmacological inhibition of calpain or caspase-3 prevented this casting-induced atrophy. Interestingly, inhibition of calpain activity also prevented caspase-3 activation, and, conversely, inhibition of caspase-3 prevented calpain activation. These findings indicate that a regulatory cross talk exists between these proteases and provide the first evidence that the activation of calpain and caspase-3 is required for inactivity-induced limb muscle atrophy.

Download Full-text

Muscle Atrophy After ACL Injury: Implications for Clinical Practice

Sports Health A Multidisciplinary Approach ◽

10.1177/1941738120944256 ◽

2020 ◽

Vol 12 (6) ◽

pp. 579-586

Author(s):

Lindsey K. Lepley ◽

Steven M. Davi ◽

Julie P. Burland ◽

Adam S. Lepley

Keyword(s):

Clinical Review ◽

Muscle Mass ◽

Muscle Atrophy ◽

Cruciate Ligament ◽

Muscle Loss ◽

Disuse Atrophy ◽

Tissue Quality ◽

Level Of Evidence ◽

Joint Injury ◽

Inducing Factors

Context: Distinct from the muscle atrophy that develops from inactivity or disuse, atrophy that occurs after traumatic joint injury continues despite the patient being actively engaged in exercise. Recognizing the multitude of factors and cascade of events that are present and negatively influence the regulation of muscle mass after traumatic joint injury will likely enable clinicians to design more effective treatment strategies. To provide sports medicine practitioners with the best strategies to optimize muscle mass, the purpose of this clinical review is to discuss the predominant mechanisms that control muscle atrophy for disuse and posttraumatic scenarios, and to highlight how they differ. Evidence Acquisition: Articles that reported on disuse atrophy and muscle atrophy after traumatic joint injury were collected from peer-reviewed sources available on PubMed (2000 through December 2019). Search terms included the following: disuse muscle atrophy OR disuse muscle mass OR anterior cruciate ligament OR ACL AND mechanism OR muscle loss OR atrophy OR neurological disruption OR rehabilitation OR exercise. Study Design: Clinical review. Level of Evidence: Level 5. Results: We highlight that (1) muscle atrophy after traumatic joint injury is due to a broad range of atrophy-inducing factors that are resistant to standard resistance exercises and need to be effectively targeted with treatments and (2) neurological disruptions after traumatic joint injury uncouple the nervous system from muscle tissue, contributing to a more complex manifestation of muscle loss as well as degraded tissue quality. Conclusion: Atrophy occurring after traumatic joint injury is distinctly different from the muscle atrophy that develops from disuse and is likely due to the broad range of atrophy-inducing factors that are present after injury. Clinicians must challenge the standard prescriptive approach to combating muscle atrophy from simply prescribing physical activity to targeting the neurophysiological origins of muscle atrophy after traumatic joint injury.

Download Full-text

The ubiquitin proteasome system in atrophying skeletal muscle: roles and regulation

AJP Cell Physiology ◽

10.1152/ajpcell.00125.2016 ◽

2016 ◽

Vol 311 (3) ◽

pp. C392-C403 ◽

Cited By ~ 57

Author(s):

Philippe A. Bilodeau ◽

Erin S. Coyne ◽

Simon S. Wing

Keyword(s):

Signaling Pathways ◽

Muscle Atrophy ◽

Molecular Mechanisms ◽

Muscle Wasting ◽

Clinical Problem ◽

Ubiquitin Proteasome System ◽

Mechanisms Of Action ◽

Loss Of Function ◽

Critical Determinant ◽

Ubiquitin Proteasome

Muscle atrophy complicates many diseases as well as aging, and its presence predicts both decreased quality of life and survival. Much work has been conducted to define the molecular mechanisms involved in maintaining protein homeostasis in muscle. To date, the ubiquitin proteasome system (UPS) has been shown to play an important role in mediating muscle wasting. In this review, we have collated the enzymes in the UPS whose roles in muscle wasting have been confirmed through loss-of-function studies. We have integrated information on their mechanisms of action to create a model of how they work together to produce muscle atrophy. These enzymes are involved in promoting myofibrillar disassembly and degradation, activation of autophagy, inhibition of myogenesis as well as in modulating the signaling pathways that control these processes. Many anabolic and catabolic signaling pathways are involved in regulating these UPS genes, but none appear to coordinately regulate a large number of these genes. A number of catabolic signaling pathways appear to instead function by inhibition of the insulin/IGF-I/protein kinase B anabolic pathway. This pathway is a critical determinant of muscle mass, since it can suppress key ubiquitin ligases and autophagy, activate protein synthesis, and promote myogenesis through its downstream mediators such as forkhead box O, mammalian target of rapamycin, and GSK3β, respectively. Although much progress has been made, a more complete inventory of the UPS genes involved in mediating muscle atrophy, their mechanisms of action, and their regulation will be useful for identifying novel therapeutic approaches to this important clinical problem.

Download Full-text

Nutritional strategies to counteract muscle atrophy caused by disuse and to improve recovery

Nutrition Research Reviews ◽

10.1017/s0954422413000115 ◽

2013 ◽

Vol 26 (2) ◽

pp. 149-165 ◽

Cited By ~ 35

Author(s):

Hugues Magne ◽

Isabelle Savary-Auzeloux ◽

Didier Rémond ◽

Dominique Dardevet

Keyword(s):

Mass Loss ◽

Muscle Mass ◽

Muscle Atrophy ◽

Whey Proteins ◽

Leucine Supplementation ◽

Positive Effects ◽

Muscle Disuse ◽

Muscle Mass Loss ◽

Nutritional Strategies ◽

Mass Recovery

Periods of immobilisation are often associated with pathologies and/or ageing. These periods of muscle disuse induce muscle atrophy which could worsen the pathology or elderly frailty. If muscle mass loss has positive effects in the short term, a sustained/uncontrolled muscle mass loss is deleterious for health. Muscle mass recovery following immobilisation-induced atrophy could be critical, particularly when it is uncompleted as observed during ageing. Exercise, the best way to recover muscle mass, is not always applicable. So, other approaches such as nutritional strategies are needed to limit muscle wasting and to improve muscle mass recovery in such situations. The present review discusses mechanisms involved in muscle atrophy following disuse and during recovery and emphasises the effect of age in these mechanisms. In addition, the efficiency of nutritional strategies proposed to limit muscle mass loss during disuse and to improve protein gain during recovery (leucine supplementation, whey proteins, antioxidants and anti-inflammatory compounds, energy intake) is also discussed.

Download Full-text