Mitochondrial Carbonic Anhydrase VA Deficiency Resulting from CA5A Alterations Presents with Hyperammonemia in Early Childhood

Karnebeek, Clara D. van; Sly, William S.; Ross, Colin J.D.; Salvarinova, Ramona; Yaplito‐Lee, Joy; Santra, Saikat; Shyr, Casper; Horvath, Gabriella; Eydoux, Patrice; Lehman, Anna; Bernard, Virginie; Newlove, Theresa; Ukpeh, Henry; Chakrapani, Anupam; Preece, Mary Anne; Ball, Sarah; Pitt, James; Vallance, Hilary; Coulter‐Mackie, Marion B.; Nguyen, Hien Anh; Zhang, Linhua; Bhavsar, Amit P.; Sinclair, Graham; Waheed, Abdül; Wasserman, Wyeth W.; Stöckler‐Ipsiroglu, Sylvia

doi:10.1016/j.ajhg.2014.01.006

Cited by 83 publications

(77 citation statements)

References 25 publications

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“…Trio whole exome sequencing (WES) was carried out to exclude any novel genetic defects in the biotin pathway, and included analyses for any mutations in the mitochondrial carbonic anhydrase VA (CA5A) gene which presents with MCD phenotype (Karnebeek et al 2014) but all tests were non-contributory.…”

Section: Case Reportmentioning

confidence: 99%

Leigh-Like Syndrome Due to Homoplasmic m.8993T>G Variant with Hypocitrullinemia and Unusual Biochemical Features Suggestive of Multiple Carboxylase Deficiency (MCD)

et al. 2016

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Leigh syndrome (LS), or subacute necrotizing encephalomyelopathy, is a genetically heterogeneous, relentlessly progressive, devastating neurodegenerative disorder that usually presents in infancy or early childhood. A diagnosis of Leigh-like syndrome may be considered in individuals who do not fulfil the stringent diagnostic criteria but have features resembling Leigh syndrome.We describe a unique presentation of Leigh-like syndrome in a 3-year-old boy with elevated 3-hydroxyisovalerylcarnitine (C5-OH) on newborn screening (NBS).Subsequent persistent plasma elevations of C5-OH and propionylcarnitine (C3) as well as fluctuating urinary markers were suggestive of multiple carboxylase deficiency (MCD). Normal enzymology and mutational analysis of genes encoding holocarboxylase synthetase (HLCS) and biotinidase (BTD) excluded MCD. Biotin uptake studies were normal excluding biotin transporter deficiency. His clinical features at 13 months of age comprised psychomotor delay, central hypotonia, myopathy, failure to thrive, hypocitrullinemia, recurrent episodes of decompensation with metabolic keto-lactic acidosis and an episode of hyperammonemia. Biotin treatment from 13 months of age was associated with increased patient activity, alertness,

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Section: Case Reportmentioning

confidence: 99%

Leigh-Like Syndrome Due to Homoplasmic m.8993T>G Variant with Hypocitrullinemia and Unusual Biochemical Features Suggestive of Multiple Carboxylase Deficiency (MCD)

et al. 2016

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“…The first discovery was a homozygous missense variant in CA5A (Mendelian Inheritance in Man [MIM] number 114761), encoding mitochondrial carbonic anhydrase VA, which is pivotal to the function of mitochondrial enzymes. 17 Our group reported that a deficiency in this enzyme causes neonatal hyperammonemia, hyperlactatemia, and hypoglycemia. 17 Such a deficiency is amenable to treatment with carglumic acid and an emergency protocol, which can prevent irreversible neurologic sequelae.…”

Section: Resultsmentioning

confidence: 96%

“…17 Our group reported that a deficiency in this enzyme causes neonatal hyperammonemia, hyperlactatemia, and hypoglycemia. 17 Such a deficiency is amenable to treatment with carglumic acid and an emergency protocol, which can prevent irreversible neurologic sequelae. We added this condition to the two-tiered diagnostic algorithm and interactive tool at Treatable ID.org (freely available as native and Web applications at www.treatable-id.org) to support clinicians in early identification.…”

Section: Resultsmentioning

confidence: 96%

Exome Sequencing and the Management of Neurometabolic Disorders

et al. 2016

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BACKGROUND Whole-exome sequencing has transformed gene discovery and diagnosis in rare diseases. Translation into disease-modifying treatments is challenging, particularly for intellectual developmental disorder. However, the exception is inborn errors of metabolism, since many of these disorders are responsive to therapy that targets pathophysiological features at the molecular or cellular level. METHODS To uncover the genetic basis of potentially treatable inborn errors of metabolism, we combined deep clinical phenotyping (the comprehensive characterization of the discrete components of a patient’s clinical and biochemical phenotype) with whole-exome sequencing analysis through a semiautomated bioinformatics pipeline in consecutively enrolled patients with intellectual developmental disorder and unexplained metabolic phenotypes. RESULTS We performed whole-exome sequencing on samples obtained from 47 probands. Of these patients, 6 were excluded, including 1 who withdrew from the study. The remaining 41 probands had been born to predominantly nonconsanguineous parents of European descent. In 37 probands, we identified variants in 2 genes newly implicated in disease, 9 candidate genes, 22 known genes with newly identified phenotypes, and 9 genes with expected phenotypes; in most of the genes, the variants were classified as either pathogenic or probably pathogenic. Complex phenotypes of patients in five families were explained by coexisting monogenic conditions. We obtained a diagnosis in 28 of 41 probands (68%) who were evaluated. A test of a targeted intervention was performed in 18 patients (44%). CONCLUSIONS Deep phenotyping and whole-exome sequencing in 41 probands with intellectual developmental disorder and unexplained metabolic abnormalities led to a diagnosis in 68%, the identification of 11 candidate genes newly implicated in neurometabolic disease, and a change in treatment beyond genetic counseling in 44%. (Funded by BC Children’s Hospital Foundation and others.)

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“…Patients with a mutation in CA12 exhibit hyponatremia and hyperchlorhydria [34]. Individuals with homozygous mutation in CA5a are reported to have lethargy, hyperlactatemia, and hyperammonemia during the neonatal period and early childhood [35]. CA6 is initially described as a gustatory protein and highly expressed in the salivary and mammary glands.…”

Section: Introductionmentioning

confidence: 99%

Expression of Carbonic Anhydrase I in Motor Neurons and Alterations in ALS

Liu

Bowser

et al. 2016

IJMS

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Carbonic anhydrase I (CA1) is the cytosolic isoform of mammalian α-CA family members which are responsible for maintaining pH homeostasis in the physiology and pathology of organisms. A subset of CA isoforms are known to be expressed and function in the central nervous system (CNS). CA1 has not been extensively characterized in the CNS. In this study, we demonstrate that CA1 is expressed in the motor neurons in human spinal cord. Unexpectedly, a subpopulation of CA1 appears to be associated with endoplasmic reticulum (ER) membranes. In addition, the membrane-associated CA1s are preferentially upregulated in amyotrophic lateral sclerosis (ALS) and exhibit altered distribution in motor neurons. Furthermore, long-term expression of CA1 in mammalian cells activates apoptosis. Our results suggest a previously unknown role for CA1 function in the CNS and its potential involvement in motor neuron degeneration in ALS.

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Mitochondrial Carbonic Anhydrase VA Deficiency Resulting from CA5A Alterations Presents with Hyperammonemia in Early Childhood

Cited by 83 publications

References 25 publications

Leigh-Like Syndrome Due to Homoplasmic m.8993T>G Variant with Hypocitrullinemia and Unusual Biochemical Features Suggestive of Multiple Carboxylase Deficiency (MCD)

Leigh-Like Syndrome Due to Homoplasmic m.8993T>G Variant with Hypocitrullinemia and Unusual Biochemical Features Suggestive of Multiple Carboxylase Deficiency (MCD)

Exome Sequencing and the Management of Neurometabolic Disorders

Expression of Carbonic Anhydrase I in Motor Neurons and Alterations in ALS

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