AGC1 Deficiency Associated with Global Cerebral Hypomyelination

Wibom, Rolf; Lasorsa, Francesco M.; Töhönen, Virpi; Barbaro, Michela; Sterky, Fredrik; Kucinski, Thomas; Naess, K; Jönsson, Malin; Pierri, Ciro Leonardo; Palmieri, Ferdinando; Wedell, Anna

doi:10.1056/nejmoa0900591

Cited by 142 publications

(168 citation statements)

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“…2d), the glutamate carrier, and also in many other mitochondrial carrier subfamilies, thereby confirming its importance in the function and/or structure of mitochondrial carriers rather than in substrate binding (Palmieri 2013). The Arg353Gln mutation occurs in a different domain of the AGC1 transporter from the Gln590Arg mutation that was previously reported in one subject (Wibom et al 2009). The Gln590Arg mutation involves an amino acid residue that protrudes into the internal cavity of the AGC1 carrier immediately above the substrate binding site (Wibom et al 2009).…”

Section: Resultssupporting

confidence: 63%

“…The Arg353Gln mutation occurs in a different domain of the AGC1 transporter from the Gln590Arg mutation that was previously reported in one subject (Wibom et al 2009). The Gln590Arg mutation involves an amino acid residue that protrudes into the internal cavity of the AGC1 carrier immediately above the substrate binding site (Wibom et al 2009). In contrast, the Arg353Gln mutation involves an amino acid residue that is located just below the m-gate of the carrier and is thought to participate in closing and opening the carrier on the matrix side through an interaction with a highly conserved glutamate at residue 384 ( Fig.…”

Section: Resultsmentioning

confidence: 59%

“…The myelination defect primarily stems from neuronal loss attributable to the energy deficit caused by a lack of cellular reducing equivalents generated by the glutamate-aspartate shuttle (Wolf and van der Knaap 2009). The brain insult is possibly compounded by a lack of neuronal-generated NAA that is required as a precursor by oligodendrocytes to synthesize myelin and would lead to the secondary hypomyelination also observed in these patients (Wibom et al 2009). As reduced NAA can be indicative of either decreased NAA production or neuronal loss, it is not possible to discern which mechanism predominates in AGC1 deficiency.…”

Section: Discussionmentioning

confidence: 96%

“…Indeed, this is only the second report of autosomal recessive SLC25A12 mutations causing severe neurologic disease. The initial 2009 report linking SLC25A12 to neurologic disease involved a Swedish girl who was found by candidate gene sequencing to harbor a homozygous AGC1 mutation that caused infantile-onset severe psychomotor retardation, hypotonia, epilepsy, global cerebral hypomyelination, and dramatically decreased NAA (Wibom et al 2009). SLC25A12 encodes a neuronal-specific mitochondrial aspartate-glutamate carrier (aspartate-glutamate carrier isoform 1, AGC1).…”

Section: Discussionmentioning

confidence: 99%

“…A distinct disorder, AGC2 deficiency, results from SLC25A13 mutations that reduce aspartate-glutamate carrier isoform 2 (AGC2) function with impaired malate/aspartate shuttle activity in the liver (Saheki and Kobayashi 2002). The prior report in the Swedish infant demonstrated complete loss of recombinant mutant AGC1 activity, resulting in no transport of aspartate or glutamate even after a 60 min incubation period (Wibom et al 2009). In contrast, the homozygous c.1058G>A missense mutation identified in this consanguineous Indian family reduces recombinant mutant AGC1 activity to approximately 15 % of the initial wild-type rate, as determined when measuring either aspartate transport or glutamate transport.…”

Section: Discussionmentioning

confidence: 99%

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AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

et al. 2014

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Background: Whole exome sequencing (WES) offers a powerful diagnostic tool to rapidly and efficiently sequence all coding genes in individuals presenting for consideration of phenotypically and genetically heterogeneous disorders such as suspected mitochondrial disease. Here, we report results of WES and functional validation in a consanguineous Indian kindred where two siblings presented with profound developmental delay, congenital hypotonia, refractory epilepsy, abnormal myelination, fluctuating basal ganglia changes, cerebral atrophy, and reduced N-acetylaspartate (NAA).Methods: Whole blood DNA from one affected and one unaffected sibling was captured by Agilent SureSelect Human All Exon kit and sequenced on the Illumina HiSeq2000. Mutations were validated by Sanger sequencing

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Section: Resultssupporting

confidence: 63%

Section: Resultsmentioning

confidence: 59%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

et al. 2014

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Mitochondrial Carriers

Arco

Satrústegui

2013

Encyclopedia of Life Sciences

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In eukaryotic cells, the exchange of metabolites across the inner mitochondrial membrane is performed by members of the mitochondrial carrier family (MCF), the largest family of solute transporters. Mutations in MCF genes are associated with rare genetic diseases underscoring the relevance of individual MCF members. Mitochondrial carriers have a common tripartite structure made up by tandem repeats of 100 amino acids each containing two transmembrane α‐helices and one conserved MCF signature. MCF members are present in two states, c and m, with binding sites for substrates facing either the intermembrane (c) or matrix (m) space. X‐ray crystallography of the mitochondrial ADP/ATP carrier in the c‐state has shown that the six α‐helices form a compact bundle shaping a cavity sealed on the matrix side by a salt‐bridge network. Substrate binding perturbs the salt‐bridge network triggering conformational changes that cause the opening of the carrier towards the matrix coupled to substrate transport. Key Concepts: Mitochondrial carriers perform the exchange of metabolites, nucleotides and cofactors through the inner mitochondrial membrane. Mitochondrial carriers form an evolutionary conserved family present in all eukaryotic cells. Mitochondrial carriers share a tripartite structure made up by repeats of 100 amino acids containing two α‐helices connected by a hydrophilic loop. Phylogenetic analyses have shown the existence of a limited number of mitochondrial carrier subfamilies involved in the transport of structurally related substrates. Mutations in nine mitochondrial carriers cause autosomal recessive disorders in humans. Mitochondrial carriers are present in either one of two different states, c and m, in which binding sites for substrates face the intermembrane (c) or matrix (m) spaces. During the transport cycle, substrate binding in each of these states induces a transition to the other state which is coupled to substrate transport. The three‐dimensional structure solved for the ADP/ATP carrier in the c state is consistent with a bundle of six transmembrane α‐helices forming an aqueous cavity closed towards the matrix by electrostatic interactions. Specific interactions of substrates with the substrate‐binding site within the aqueous cavity will disturb the electrostatic interactions that maintain the carrier closed to the matrix side. Substrate translocation by mitochondrial carriers occurs coupled to conformational movements of the α‐helices that open the carrier.

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Manifestations of Drug Toxicity on Mitochondria in the Nervous System

Prehn

Llorente‐Folch

2018

Mitochondrial Dysfunction Caused by Drugs and Environmental Toxicants

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AGC1 Deficiency Associated with Global Cerebral Hypomyelination

Cited by 142 publications

References 19 publications

AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

Mitochondrial Carriers

Manifestations of Drug Toxicity on Mitochondria in the Nervous System

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