Missense mutations in desmin associated with familial cardiac and skeletal myopathy

Goldfarb, Lev G.; Park, Kye-Yoon; Červen̆áková, Larisa; Gorokhova, Svetlana; Lee, Hee-Suk; Vasconcelos, Olavo M.; Nagle, James W.; Semino–Mora, Cristina; Sivakumar, Kumaraswamy; Dalakas, Marinos C.

doi:10.1038/1300

Cited by 461 publications

(304 citation statements)

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“…40 Indeed, in a family segregating both p.Ala360Pro and p.Asn393Ile mutations, a highly aggressive early onset cardioskeletal myopathy affected only those having both mutations in a compound heterozygous fashion but spared the carriers of either mutation. 9 The p.Ala337Pro, p.Leu338Arg, p.Asp399Tyr, p.Glu401Lys and p.Arg406Trp mutations alone make desmin filaments dysfunctional and cause increasingly more severe disease that starts earlier and leads to the development of life-threatening dysphagia, cardiomyopathy, or respiratory weakness. 40 The severity of illness caused by the mutations located in the C-terminal part of the 2B alphahelical domain can be explained by structural relationships these mutations potentially disrupt.…”

Section: Mutations In the 2b Des Segmentmentioning

confidence: 99%

“…9 They presented with syncopal episodes and complete heart block requiring insertion of a permanent pacemaker at the age of 2, 9 and 10 years. EchoCG showed moderate to severe biatrial dilatation but normal ventricle size.…”

Section: Disease Severity In Patients With Autosomal Recessive Inherimentioning

confidence: 99%

“…Misfolded desmin resists turnover by the cellular enzymatic machinery. 7 Identification of multiple causative mutations in the DES gene 6,[9][10][11] helped to establish desminopathy as a distinct disease. The second genetically independent subset of desminopathy is myopathy associated with mutations in CRYAB, a chaperone that normally stabilizes proteins including desmin and prevents their irreversible aggregation.…”

Section: Introductionmentioning

confidence: 99%

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Intermediate Filament Diseases: Desminopathy

Goldfarb

Olivé

Vicart³

et al. 2008

Advances in Experimental Medicine and Biology

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104

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Desminopathy is one of the most common intermediate filament human disorders associated with mutations in closely interacting proteins, desmin and alphaB-crystallin. The inheritance pattern in familial desminopathy is characterized as autosomal dominant or autosomal recessive, but many cases have no family history. At least some and likely most sporadic desminopathy cases are associated with de novo DES mutations. The age of disease onset and rate of progression may vary depending on the type of inheritance and location of the causative mutation. Typically, the illness presents with lower and later upper limb muscle weakness slowly spreading to involve truncal, neckflexor, facial and bulbar muscles. Skeletal myopathy is often combined with cardiomyopathy manifested by conduction blocks, arrhythmias and chronic heart failure resulting in premature sudden death. Respiratory muscle weakness is a major complication in some patients. Sections of the affected skeletal and cardiac muscles show abnormal fibre areas containing chimeric aggregates consisting of desmin and other cytoskeletal proteins. Various DES gene mutations: point mutations, an insertion, small in-frame deletions and a larger exon-skipping deletion, have been identified in desminopathy patients. The majority of these mutations are located in conserved alpha-helical segments, but additional mutations have recently been identified in the tail domain. Filament and network assembly studies indicate that most but not all disease-causing mutations make desmin assembly-incompetent and able to disrupt a pre-existing filamentous network in dominant-negative fashion. AlphaBcrystallin serves as a chaperone for desmin preventing its aggregation under various forms of stress; mutant CRYAB causes cardiac and skeletal myopathies identical to those resulting from DES mutations.

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Section: Mutations In the 2b Des Segmentmentioning

confidence: 99%

Section: Disease Severity In Patients With Autosomal Recessive Inherimentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Intermediate Filament Diseases: Desminopathy

Goldfarb

Olivé

Vicart³

et al. 2008

Advances in Experimental Medicine and Biology

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104

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“…The mutant desmin transgenic mouse (D7‐Des Tg) carries a 7 amino acid deletion R172‐E178 in DES and provides a clinically relevant mouse model of cardiac proteotoxicity 9, 10, 11, 12. This model manifests a collapse of the desmin network, and accumulation of desmin aggregates, which contributes to cardiomyopathy 10.…”

Section: Introductionmentioning

confidence: 99%

Aberrant Mitochondrial Fission Is Maladaptive in Desmin Mutation–Induced Cardiac Proteotoxicity

Alam

Abdullah

Aishwarya

et al. 2018

JAHA

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BackgroundDesmin filament proteins interlink the contractile myofibrillar apparatus with mitochondria, nuclei and the sarcolemma. Mutations in the human desmin gene cause cardiac disease, remodeling, and heart failure but the pathophysiological mechanisms remain unknown.Methods and ResultsCardiomyocyte‐specific overexpression of mutated desmin (a 7 amino acid deletion R172‐E178, D7‐Des Tg) causes accumulations of electron‐dense aggregates and myofibrillar degeneration associated with cardiac dysfunction. Though extensive studies demonstrated that these altered ultrastructural changes cause impairment of cardiac contractility, the molecular mechanism of cardiomyocyte death remains elusive. In the present study, we report that the D7‐Des Tg mouse hearts undergo aberrant mitochondrial fission associated with increased expression of mitochondrial fission regulatory proteins. Mitochondria isolated from D7‐Des Tg hearts showed decreased mitochondrial respiration and increased apoptotic cell death. Overexpression of mutant desmin by adenoviral infection in cultured cardiomyocytes led to increased mitochondrial fission, inhibition of mitochondrial respiration, and activation of cellular toxicity. Inhibition of mitochondrial fission by mitochondrial division inhibitor mdivi‐1 significantly improved mitochondrial respiration and inhibited cellular toxicity associated with D7‐Des overexpression in cardiomyocytes.ConclusionsAberrant mitochondrial fission results in mitochondrial respiratory defects and apoptotic cell death in D7‐Des Tg hearts. Inhibition of aberrant mitochondrial fission using mitochondrial division inhibitor significantly preserved mitochondrial function and decreased apoptotic cell death. Taken together, our study shows that maladaptive aberrant mitochondrial fission causes desminopathy‐associated cellular dysfunction.

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“…76 Mutations in the desmin gene have been implicated in pathogenesis. 77 Another gene affected (mutation R120G) is named CRYAB; it encodes alpha-B-crystallin and maps to chromosome 11q21-23. 67 The product of the defective gene R120G showed decreased beta-sheet secondary structure, with reduction, or lackdepending on the substrate used in the assay-of chaperone activity in vitro.…”

Section: Desmin-related Myopathymentioning

confidence: 99%

Genetic disorders involving molecular-chaperone genes: A perspective

Macario

Grippo

Macario

2005

Genetics in Medicine

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Molecular chaperones are important for maintaining a functional set of proteins in all cellular compartments.Together with protein degradation machineries (e.g., the ubiquitin-proteasome system), chaperones form the core of the cellular protein-quality control mechanism. Chaperones are proteins, and as such, they can be affected by mutations. At least 15 disorders have been identified that are associated with mutations in genes encoding chaperones, or molecules with features suggesting that they function as chaperones. These chaperonopathies and a few other candidates are presented in this article. In most cases, the mechanisms by which the defective genes contribute to the observed phenotypes are still uncharacterized. However, the reported observations definitely

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Missense mutations in desmin associated with familial cardiac and skeletal myopathy

Cited by 461 publications

References 10 publications

Intermediate Filament Diseases: Desminopathy

Intermediate Filament Diseases: Desminopathy

Aberrant Mitochondrial Fission Is Maladaptive in Desmin Mutation–Induced Cardiac Proteotoxicity

Genetic disorders involving molecular-chaperone genes: A perspective

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