Diagnosis and Treatment of Mitochondrial Myopathies

Ahmed, Syeda; Craven, Lyndsey; Russell, Oliver M.; Turnbull, Doug M.; Vincent, Amy E.

doi:10.1007/s13311-018-00674-4

Cited by 90 publications

(91 citation statements)

References 74 publications

(67 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Rational diet therapy (usually, ketogenic diet) with a reduced amount of easily digestible carbohydrates, high fat content and average protein content in combination with exercise therapy is recommended to be used [2,65].…”

Section: Therapy For Mitochondrial Dysfunctionsmentioning

confidence: 99%

“…The possibility of mitochondrial replacement therapy in 5 main areas is studied: 1 -xenotopic gene expression; 2 -allotopic gene expression [25]; 3 -the synthesis of artificially created in vivo mitochondrial tRNA and rRNA with their subsequent transfer to mutant mitochondria with damaged structures replacement; 4 -the creation of "vector" nucleic acids complementary to the mutated piece of mtDNA, which while binding to them, contribute to their inhibition and shutdown of the replication processes; 5 -the use of artificially created vesicles penetrating through the membranes of mitochondria and restoring lost functions. Besides, the mutation correction systems in mtDNA based on molecular genome editing technologies, for example, systems called "mitochondrial zinc fingers", mitoTALEN, mitoCRISPR/Cas9 are being developed [2,11]. The main disadvantage of these directions is that they do not eliminate the underlying mutation in the mitochondria genome, but only reduce the heteroplasmy level, resulting in partial restoration of the mitochondria function.…”

Section: Therapy For Mitochondrial Dysfunctionsmentioning

confidence: 99%

“…The direction determining the significance and role of energy exchange disorders in mitochondria in the pathogenesis of diseases is developing actively in medical science over past decades. Тhe conception "mitochondrial dysfunctions" (MD) is formed as а result of it [2,4,67].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Mitochondrial dysfunctions and antihypoxants

Новиков

Левченкова

Ivantsova

et al. 2020

Rev Clin Pharm Drug Ther

View full text Add to dashboard Cite

Mitochondrial dysfunctions (an impaired energy metabolism in the mitochondria) are essential in a pathogenesis of many diseases. Aim. The analysis of various mitochondrial dysfunction (MD) type study, as well as evaluation of drugs with an antihypoxic effect in their treatment. Methods. Collection, systematization and analysis of experimental and clinical data of current scientific research about the problem. Results. The mitochondrial dysfunctions can be caused by genetic disorders of the mitochondrial or nuclear genome (the primary MD or the mitochondrial diseases), as well as structural, functional and biochemical defects of mitochondria caused by other diseases (the secondary MD). MD are characterized by impaired tissue respiration, ATP synthesis deficiency and decreased energy metabolism. The clinical implications of MD are polysystemic and polymorphic. One of the biochemical sign of MD is the lactic acidosis. There are certain difficulties with the early diagnosis of primary MD. It is suggested to use complete exome sequencing among patients with a clinical suspicion on mitochondrial disease. The energotropic pharmacotherapy including drugs with an antihypoxic effect is used for MD treatment. It is more rational to use the drug combination that influences different stages of energy production. The combinations of L-carnitine, coenzyme Q10, cytochrome C and succinate-containing drugs are frequently used for MD. However, the usage of energotropic and antihypoxic drugs is not able to cure the patients and stop the progression of all disease displays. Conclusion. MD are a multidisciplinary problem, therefore, doctors of any speciality must be competent in the MD diagnosis and treatment. The use of energotropic agents in the MD treatment requires further research. Numerous issues remain open (daily drug doses choice, treatment duration, rational combinations). The phenotype variability and the uniqueness of diagnosed cases, clinical and genetic differences between patient groups with mitochondrial diseases fail to create homogeneous samplings for therapy effectiveness and safety analysis. The literature data are the results of different degrees of reliability. The international efforts are needed to unify studies of related mitochondrial disorders, which, in combination with a constant improvement of MD pathogenesis knowledge will allow to develop more effective treatment regimens.

show abstract

Section: Therapy For Mitochondrial Dysfunctionsmentioning

confidence: 99%

Section: Therapy For Mitochondrial Dysfunctionsmentioning

confidence: 99%

See 1 more Smart Citation

Mitochondrial dysfunctions and antihypoxants

Новиков

Левченкова

Ivantsova

et al. 2020

Rev Clin Pharm Drug Ther

View full text Add to dashboard Cite

show abstract

“…Mitochondrial myopathies (MMs), are an important group of muscle conditions characterized by isolated or predominant skeletal muscle involvement, caused primarily by the impairment of oxidative phosphorylation (OXPHOS) due to mutations of nuclear or mitochondrial DNA (1). Currently there are no available effective or disease-modifying treatments for majority of patients with mitochondrial myopathies (1). Myopathy is one of the most common manifestations of adult-onset mitochondrial disorders due to the high cellular energy demand of skeletal muscle.…”

Section: Introductionmentioning

confidence: 99%

Clinical Profile and Outcome of Pediatric Mitochondrial Myopathy in China

Zhao

et al. 2020

Front. Neurol.

View full text Add to dashboard Cite

Introduction: Mitochondrial myopathy in children has notable clinical and genetic heterogeneity, but detailed data is lacking. Patients and Methods: In this study, we retrospectively reviewed the clinical presentation, laboratory investigation, genetic and histopathological characteristics, and follow-ups of 21 pediatric mitochondrial myopathy cases from China. Results: Twenty-four patients suspected with mitochondrial myopathy were enrolled initially and 21 were genetically identified. Fourteen patients were found to harbor mitochondrial DNA point mutations (14/21, 66.7%), including m.3243A>G (9/15, 60%), m.3303C>T (2/15, 13.3%), m.3302A>G (1/15, 6.7%), m.3250T>C (1/15, 6.7%), m.3251A>G (1/15, 6.7%), of whom 12 patients presented with progressive proximal mitochondrial myopathy (12/14, 85.7%). Three patients revealed large-scale deletion in blood or muscle tissue (3/21, 14.3%), presenting with Kearns-Sayer syndrome (1/3, 33.3%) or chronic progressive external ophthalmoplegia (2/3, 66.7%). Four patients were found to harbor pathogenic nuclear gene variants (4/21, 19.0%), including five variants in TK2 gene and two variants in SURF1 gene. During the follow-ups up to 7 years, 10 patients developed cardiomyopathy (10/21, 47.6%), 13 patients occurred at least once hypercapnic respiratory failure (13/21, 61.9%), six experienced recurrent respiratory failure and intubation (6/21, 28.6%), eight patients failed to survive (8/21, 38.1%). With nocturnal non-invasive ventilation of BiPAP, three patients recovered from respiratory failure, and led a relative stable and functional life (3/21, 14.3%). Conclusion: Mitochondrial myopathy in children has great clinical, pathological, and genetical heterogeneity. Progressive proximal myopathy is most prevalent. Mitochondrial DNA point mutations are most common. And respiratory failure is a critical risk factor of poor prognosis.

show abstract

“…Mutations in nuclear DNA or mitochondrial DNA (mtDNA) can disrupt the function of mitochondrial proteins resulting in an impairment of oxidative phosphorylation that may cause damage not only to skeletal muscle, but to other organs as well. Although no curative therapies are yet available, Ahmed et al discuss strategies for the symptomatic management of these diseases [11]. A recent success in the field has been the availability of new reproductive options that may prevent the transmission of disease-causing mutations from mother to offspring.…”

mentioning

confidence: 99%