Combined malonic and methylmalonic aciduria: exome sequencing reveals mutations in the ACSF3 gene in patients with a non-classic phenotype

Alfares, Ahmed; Nunez, Laura Dempsey; Al‐Thihli, Khalid; Mitchell, John; Mélancon, Serge B.; Anastasio, Natascia; Ha, Kevin C.H.; Majewski, Jacek; Rosenblatt, David S.; Braverman, Nancy

doi:10.1136/jmedgenet-2011-100230

Cited by 42 publications

(50 citation statements)

References 27 publications

(20 reference statements)

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“…Although the relative contributions of each of these potential sources of mitochondrial malonate remains to be determined, our model describes the roles for ACSF3 and MLYCD in regulating mitochondrial malonate concentrations. Consistent with our model, mutations in human ACSF3 or MLYCD result in toxic accumulation of malonate and systemic metabolic acidosis (Alfares et al, 2011; Sloan et al, 2011). …”

Section: Discussionsupporting

confidence: 84%

“…The severe malonic and methylmalonic aciduria characteristic of MLYCD deficiency is also accompanied by developmental delay, seizure disorders, hypoglycemia, and cardiomyopathy. Recently, patients that presented with combined malonic and methylmalonic aciduria without mutations in MLYCD were found to have nonsynonymous mutations in the ACSF3 gene (Alfares et al, 2011; Sloan et al, 2011). The similarities in the phenotypes of MLYCD and ACSF3 deficiencies suggest that they exist in the same biochemical pathway.…”

Section: Introductionmentioning

confidence: 99%

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The Mammalian Malonyl-CoA Synthetase ACSF3 Is Required for Mitochondrial Protein Malonylation and Metabolic Efficiency

Bowman

Rodriguez

Alpergin

et al. 2017

Cell Chemical Biology

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Summary Malonyl-CoA is a central metabolite in mammalian fatty acid biochemistry generated and utilized in the cytoplasm; however, little is known about noncanonical organelle-specific malonyl-CoA metabolism. Intramitochondrial malonyl-CoA is generated by a malonyl-CoA synthetase, ACSF3, that produces malonyl-CoA from malonate, an endogenous competitive inhibitor of succinate dehydrogenase. To determine the metabolic requirement for mitochondrial malonyl-CoA, ACSF3 knockout (KO) cells were generated by CRISPR/Cas-mediated genome editing. ACSF3 KO cells exhibited elevated malonate and impaired mitochondrial metabolism. Unbiased and targeted metabolomics analysis of KO and control cells in the presence or absence of exogenous malonate revealed metabolic changes dependent on either malonate or malonyl-CoA. While ACSF3 was required for the metabolism and therefore detoxification of malonate, ACSF3-derived malonyl-CoA was specifically required for lysine malonylation of mitochondrial proteins. Together, these data describe an essential role for ACSF3 in dictating the metabolic fate of mitochondrial malonate and malonyl-CoA in mammalian metabolism.

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Section: Discussionsupporting

confidence: 84%

Section: Introductionmentioning

confidence: 99%

The Mammalian Malonyl-CoA Synthetase ACSF3 Is Required for Mitochondrial Protein Malonylation and Metabolic Efficiency

Bowman

Rodriguez

Alpergin

et al. 2017

Cell Chemical Biology

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“…We therefore turned to exome sequencing to identify the gene affected in this patient. This procedure has proven to be an effective tool for disease gene identification in rare autosomal recessive disorders with limited number of affected individuals [12]. In this case, gene identification by exome sequencing was successful with a single patient.…”

Section: Discussionmentioning

confidence: 94%

“…(3) The annotation of variants was performed by ANNOVAR [11] for the type of mutations, presence in dbSNP132, minor allele frequency in the 1000 Genomes project, EVS (Exome variant server), SIFT, Polyphen-2 and PHASTCONS scores. (4) Novel variants were defined as those having an allele frequency of less than 0.05 in the 1000 Genomes Project and predicted to be non-synonymous substitutions caused by missense and nonsense single-nucleotide polymorphisms (SNP), splice-site SNPs, and frame shift changes due to indels [12]. Candidate genes containing either a homozygous or two potentially compound heterozygous variants were selected for further study and were manually examined using IGV [13].…”

Section: Exome Sequencingmentioning

confidence: 99%

Late onset of symptoms in an atypical patient with the cblJ inborn error of vitamin B12 metabolism: Diagnosis and novel mutation revealed by exome sequencing

Kim

Lee

Hwu

et al. 2012

Molecular Genetics and Metabolism

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“…Defects in other genes within the propionate catabolism pathway or mitochondrial disorders may also result in excretion of methylmalonic acid in the urine [89, 90]. These disorders are rarer than classical isolated MMA, often manifest other biochemically diagnostic markers in urine or plasma to suggest the diagnosis, and will not be addressed further in this review.…”

Section: Diagnosismentioning

confidence: 99%

Methylmalonic and propionic acidemias: clinical management update

Fraser

Venditti

2016

Current Opinion in Pediatrics

162

163

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Purpose of review Recent clinical studies and management guidelines for the treatment of the organic acidopathies methylmalonic acidemia (MMA) and propionic acidemia (PA) address the scope of interventions to maximize health and quality of life. Unfortunately, these disorders continue to cause significant morbidity and mortality due to acute and chronic systemic and end-organ injury. Recent findings Dietary management with medical foods has been a mainstay of therapy for decades, yet well controlled patients can manifest growth, development, cardiac, ophthalmological, renal and neurological complications. Patients with organic acidopathies suffer metabolic brain injury which targets specific regions of the basal ganglia in a distinctive pattern, and these injuries may occur even with optimal management during metabolic stress. Liver transplantation has improved quality of life and metabolic stability, yet transplantation in this population does not entirely prevent brain injury or the development of optic neuropathy and cardiac disease. Summary Management guidelines should identify necessary screening for patients with MMA and PA, and improve anticipatory management of progressive end-organ disease. Liver transplantation improves overall metabolic control, but injury to non-regenerative tissues may not be mitigated. Continued use of medical foods in these patients requires prospective studies to demonstrate evidence of benefit in a controlled manner.

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Combined malonic and methylmalonic aciduria: exome sequencing reveals mutations in the ACSF3 gene in patients with a non-classic phenotype

Cited by 42 publications

References 27 publications

The Mammalian Malonyl-CoA Synthetase ACSF3 Is Required for Mitochondrial Protein Malonylation and Metabolic Efficiency

The Mammalian Malonyl-CoA Synthetase ACSF3 Is Required for Mitochondrial Protein Malonylation and Metabolic Efficiency

Late onset of symptoms in an atypical patient with the cblJ inborn error of vitamin B12 metabolism: Diagnosis and novel mutation revealed by exome sequencing

Methylmalonic and propionic acidemias: clinical management update

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