Common Pathogenic Mechanisms in Centronuclear and Myotubular Myopathies and Latest Treatment Advances

Gómez-Oca, Raquel; Cowling, Belinda S.; Laporte, Jocelyn

doi:10.3390/ijms222111377

Cited by 23 publications

(24 citation statements)

References 264 publications

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“…Although it is easy to understand that mutations in RYR1 or CACNA1S can be found in patients with MH or CCD and that mutations in STIM1 or ORAI1 are associated with TAM/Stormorken syndrome, less obvious are the cases where mutations in genes not involved in Ca 2+ -handling pathways, such as MYH7 , TTN , or MEGF10 , are detected in patients presenting with clinical symptoms and histopathological alterations like those present in RYR1- related myopathies. This apparent incongruency can be rationalized by evidence that, at least in some cases, mutations in genes apparently not directly connected with Ca 2+ signaling may indirectly affect regulation of Ca 2+ homeostasis, as proposed for SEPN1 ( Chernorudskiy et al, 2020 ) or BIN1 , MTM1 , or DNM2 ( Gómez-Oca et al, 2021 ). However, more work is needed in this direction to explain how genes not known to affect Ca 2+ signaling mat induce a myopathy.…”

Section: Discussionmentioning

confidence: 99%

“…Recessive mutations in RYR1 are the most common cause of autosomal recessive CNM, accounting for ∼15% of patients. At clinical presentation, autosomal CNM most frequently shows delayed motor milestones, nonprogressive muscle weakness and hypotonia, ptosis, ophthalmoplegia, and mild to severe respiratory impairment ( Jungbluth et al, 2008 ; Wilmshurst et al, 2010 ; Bevilacqua et al, 2011 ; Romero and Bitoun, 2011 ; Gòmez-Oca et al, 2021 ). From a histological point of view, CNM shows centralized and internalized nuclei, peripheral halos depleted of oxidative activity, and cores, although based on which gene is mutated, the histological patterns may vary ( Nicot et al, 2007 ; Bevilacqua et al, 2011 ; Gomez-Oca et al, 2021 ).…”

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

“…At clinical presentation, autosomal CNM most frequently shows delayed motor milestones, nonprogressive muscle weakness and hypotonia, ptosis, ophthalmoplegia, and mild to severe respiratory impairment ( Jungbluth et al, 2008 ; Wilmshurst et al, 2010 ; Bevilacqua et al, 2011 ; Romero and Bitoun, 2011 ; Gòmez-Oca et al, 2021 ). From a histological point of view, CNM shows centralized and internalized nuclei, peripheral halos depleted of oxidative activity, and cores, although based on which gene is mutated, the histological patterns may vary ( Nicot et al, 2007 ; Bevilacqua et al, 2011 ; Gomez-Oca et al, 2021 ). RYR1 -related CNM often presents as a mixed phenotype between CNM and core myopathies, with the presence of multiple central nuclei and core-like structures with no limited boundaries ( Abath Neto et al, 2017 ).…”

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

“…RYR1 -related CNM often presents as a mixed phenotype between CNM and core myopathies, with the presence of multiple central nuclei and core-like structures with no limited boundaries ( Abath Neto et al, 2017 ). These forms are normally caused by compound heterozygous mutations in RYR1 , where one of the two mutations usually cause premature termination of the transcript, resulting in a decrease in RYR1 protein expression levels ( Gòmez-Oca et al, 2021 ). Mutations in MTM1 account for >50% of CNM cases.…”

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

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Mutations in proteins involved in E-C coupling and SOCE and congenital myopathies

Rossi

Catallo

Pierantozzi

et al. 2022

Journal of General Physiology

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In skeletal muscle, Ca2+ necessary for muscle contraction is stored and released from the sarcoplasmic reticulum (SR), a specialized form of endoplasmic reticulum through the mechanism known as excitation–contraction (E-C) coupling. Following activation of skeletal muscle contraction by the E-C coupling mechanism, replenishment of intracellular stores requires reuptake of cytosolic Ca2+ into the SR by the activity of SR Ca2+-ATPases, but also Ca2+ entry from the extracellular space, through a mechanism called store-operated calcium entry (SOCE). The fine orchestration of these processes requires several proteins, including Ca2+ channels, Ca2+ sensors, and Ca2+ buffers, as well as the active involvement of mitochondria. Mutations in genes coding for proteins participating in E-C coupling and SOCE are causative of several myopathies characterized by a wide spectrum of clinical phenotypes, a variety of histological features, and alterations in intracellular Ca2+ balance. This review summarizes current knowledge on these myopathies and discusses available knowledge on the pathogenic mechanisms of disease.

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Section: Discussionmentioning

confidence: 99%

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

Section: Ryr1 -Related Myopathiesmentioning

confidence: 99%

See 2 more Smart Citations

Mutations in proteins involved in E-C coupling and SOCE and congenital myopathies

Rossi

Catallo

Pierantozzi

et al. 2022

Journal of General Physiology

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“…BIN1 - and DNM2 -associated CNM patients show normal or slightly elevated levels of serum creatine kinase and slowly progressive muscle weakness [ 8 , 9 , 10 , 11 ]. This review will overview the functions of dynamin 2 and BIN1 in T-tubule biogenesis and discuss possible pathogenic mechanisms of CNM caused by their membrane remodelling defects, aiming for compensating other excellent reviews [ 2 , 12 , 13 , 14 , 15 , 16 ].…”

Section: Introductionmentioning

confidence: 99%

Centronuclear Myopathy Caused by Defective Membrane Remodelling of Dynamin 2 and BIN1 Variants

Fujise

Noguchi

Takeda

2022

IJMS

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Centronuclear myopathy (CNM) is a congenital myopathy characterised by centralised nuclei in skeletal myofibers. T-tubules, sarcolemmal invaginations required for excitation-contraction coupling, are disorganised in the skeletal muscles of CNM patients. Previous studies showed that various endocytic proteins are involved in T-tubule biogenesis and their dysfunction is tightly associated with CNM pathogenesis. DNM2 and BIN1 are two causative genes for CNM that encode essential membrane remodelling proteins in endocytosis, dynamin 2 and BIN1, respectively. In this review, we overview the functions of dynamin 2 and BIN1 in T-tubule biogenesis and discuss how their dysfunction in membrane remodelling leads to CNM pathogenesis.

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Integrated multi‐omics approach reveals the role of striated muscle preferentially expressed protein kinase in skeletal muscle including its relationship with myospryn complex

Li,

Lin,

Luo

et al. 2024

J cachexia sarcopenia muscle

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BackgroundAutosomal‐recessive mutations in SPEG (striated muscle preferentially expressed protein kinase) have been linked to centronuclear myopathy with or without dilated cardiomyopathy (CNM5). Loss of SPEG is associated with defective triad formation, abnormal excitation–contraction coupling, calcium mishandling and disruption of the focal adhesion complex in skeletal muscles. To elucidate the underlying molecular pathways, we have utilized multi‐omics tools and analysis to obtain a comprehensive view of the complex biological processes and molecular functions.MethodsSkeletal muscles from 2‐month‐old SPEG‐deficient (Speg‐CKO) and wild‐type (WT) mice were used for RNA sequencing (n = 4 per genotype) to profile transcriptomics and mass spectrometry (n = 4 for WT; n = 3 for Speg‐CKO mice) to profile proteomics and phosphoproteomics. In addition, interactomics was performed using the SPEG antibody on pooled muscle lysates (quadriceps, gastrocnemius and triceps) from WT and Speg‐CKO mice. Based on the multi‐omics results, we performed quantitative real‐time PCR, co‐immunoprecipitation and immunoblot to verify the findings.ResultsWe identified that SPEG interacts with myospryn complex proteins CMYA5, FSD2 and RyR1, which are critical for triad formation, and that SPEG deficiency results in myospryn complex abnormalities (protein levels decreased to 22 ± 3% for CMYA5 [P < 0.05] and 18 ± 3% for FSD2 [P < 0.01]). Furthermore, SPEG phosphorylates RyR1 at S2902 (phosphorylation level decreased to 55 ± 15% at S2902 in Speg‐CKO mice; P < 0.05), and its loss affects JPH2 phosphorylation at multiple sites (increased phosphorylation at T161 [1.90 ± 0.24‐fold], S162 [1.61 ± 0.37‐fold] and S165 [1.66 ± 0.13‐fold]; decreased phosphorylation at S228 and S231 [39 ± 6%], S234 [50 ± 12%], S593 [48 ± 3%] and S613 [66 ± 10%]; P < 0.05 for S162 and P < 0.01 for other sites). On analysing the transcriptome, the most dysregulated pathways affected by SPEG deficiency included extracellular matrix–receptor interaction (P < 1e−15) and peroxisome proliferator‐activated receptor signalling (P < 9e−14).ConclusionsWe have elucidated the critical role of SPEG in the triad as it works closely with myospryn complex proteins (CMYA5, FSD2 and RyR1), it regulates phosphorylation levels of various residues in JPH2 and S2902 in RyR1, and its deficiency is associated with dysregulation of several pathways. The study identifies unique SPEG‐interacting proteins and their phosphorylation functions and emphasizes the importance of using a multi‐omics approach to comprehensively evaluate the molecular function of proteins involved in various genetic disorders.

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Common Pathogenic Mechanisms in Centronuclear and Myotubular Myopathies and Latest Treatment Advances

Cited by 23 publications

References 264 publications

Mutations in proteins involved in E-C coupling and SOCE and congenital myopathies

Mutations in proteins involved in E-C coupling and SOCE and congenital myopathies

Centronuclear Myopathy Caused by Defective Membrane Remodelling of Dynamin 2 and BIN1 Variants

Integrated multi‐omics approach reveals the role of striated muscle preferentially expressed protein kinase in skeletal muscle including its relationship with myospryn complex

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