A Homozygous Mutation in GPT2 Associated with Nonsyndromic Intellectual Disability in a Consanguineous Family from Costa Rica

Lobo-Prada, Tanya; Sticht, Heinrich; Bogantes-Ledezma, Sixto; Ekici, Arif B.; Uebe, Steffen; Reis, André; Leal, Alejandro

doi:10.1007/8904_2016_40

Cited by 6 publications

(10 citation statements)

References 19 publications

(13 reference statements)

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“…Prior to the present report, c.1210C>T, p.Arg404* and c.815C>T, p.Pro272Leu homozygous variants in GPT2 had been reported in patients with postnatal microcephaly, IDD and progressive motor symptoms (Ouyang et al, ), another missense mutation in GPT2 , c.459 C>G p.Ser153Arg had been identified in patients with microcephaly/dolichocephaly, severe ID and motor dysfunction (Celis et al, ). A more recent study identified a novel missense GPT2 mutation, c. 286G>A p.Gly96Arg, that was linked to IDD (Lobo‐Prada et al, ). Interestingly, except for the p.Gly96Arg variant, which is only linked to IDD, all other previously reported and our patients' variants are located on the aspartate aminotransferase family domain (Figure D).…”

Section: Resultsmentioning

confidence: 99%

“…Although IDD and microcephaly are highly heterogeneous disorders, mutations in the enzyme glutamic‐pyruvic transaminase 2 ( GPT2) were recently shown to be causal genetic factors in their clinical presentation (Celis et al, ; Lobo‐Prada et al, ; Ouyang et al, ). GPT2 (also called Alanine aminotransferase; ALT2 ) localizes to mitochondria that catalyze the conversion of glutamate to α‐ketoglutarate and consequently provide energy for synaptogenesis (Yang et al, ).…”

Section: Introductionmentioning

confidence: 99%

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Novel compound heterozygous mutations in GPT2 linked to microcephaly, and intellectual developmental disability with or without spastic paraplegia

Kaymakçalan

Yarman

Goc

et al. 2017

American J of Med Genetics Pt A

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We here describe novel compound heterozygous missense variants, NM_133443:c.[400C>T] and NM_133443:[1435G>A], in the glutamic-pyruvic transaminase 2 (GPT2) gene in a large consanguineous family with two affected siblings diagnosed with microcephaly intellectual disability and developmental delay (IDD). In addition to these clinical phenotypes, the male sibling has spastic paraplegia, and the female sibling has epilepsy. Their four extended family members have IDD and microcephaly. Both of these variants, c.400C>T (p.R134C) and c.1435G>A (p.V479M), reside in the pyridoxal phosphate-dependent aminotransferase domain. The missense variants affect highly conserved amino acids and are classified to be disease-causing by meta-SVM. The candidate variants were not found in the Exome Aggregation Consortium (ExAC) dataset or in dbSNP. Both GPT2 variants have an allele frequency of 0% (0/ ∼ 600) in the whole-exome sequenced Turkish cohort. Upon Sanger sequencing, we confirmed these mutations in all affected family members and showed that the index patient and his affected sister inherited one mutant allele from each unaffected parent. To the best of our knowledge, this is the first family in which a novel compound heterozygous variant in the GPT2 gene was identified.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Novel compound heterozygous mutations in GPT2 linked to microcephaly, and intellectual developmental disability with or without spastic paraplegia

Kaymakçalan

Yarman

Goc

et al. 2017

American J of Med Genetics Pt A

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“…Recessive mutations in glutamate pyruvate transaminase 2 (GPT2) have recently been associated with intellectual disability in 5 independent families . Here we present 5 patients from 2 consanguineous families with Palestinian ancestry with a novel homozygous stop mutation in GPT2.…”

Section: Introductionmentioning

confidence: 99%

“…Recessive mutations in glutamate pyruvate transaminase 2 (GPT2) have recently been associated with intellectual disability in 5 independent families. [1][2][3][4] Here we present 5 patients from 2 consanguineous families with Palestinian ancestry with a novel homozygous stop mutation in GPT2. By comparing the common clinical features with previously published GPT2 patients the picture of a recognizable neurodevelopmental and probably neurodegenerative phenotype becomes apparent, consisting of severe IDD, spastic paraplegia, microcephaly and often epilepsy.…”

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confidence: 99%

GPT2 mutations cause developmental encephalopathy with microcephaly and features of complicated hereditary spastic paraplegia

et al. 2018

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Various genetic defects can cause intellectual and developmental disabilities (IDDs). Often IDD is a symptom of a more complex neurodevelopmental or neurodegenerative syndrome. Identifying syndromic patterns is substantive for diagnostics and for understanding the pathomechanism of a disease. Recessive glutamate pyruvate transaminase (GPT2) mutations have recently been associated with IDD in 4 families. Here, we report a novel recessive GPT2 stop mutation p.Gln24* causing a complex IDD phenotype in a homozygous state in 5 patients from 2 consanguineous Arab families. By compiling clinical information of these individuals and previously described GPT2 patients a recognizable neurodevelopmental and potentially neurodegenerative phenotype can be assigned consisting of intellectual disability, pyramidal tract affection with spastic paraplegia, microcephaly and frequently epilepsy. Because of the consistent presence of pyramidal tract affection in GPT2 patients, we further suggest that GPT2 mutations should be considered in cases with complex hereditary spastic paraplegia.

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“…It is hoped that this translational model will prove invaluable for parsing the myriad of factors (for example, developmental, genetic, environmental, neurobiological) that render an individual more susceptible to cue-motivated psychopathologies and lead to novel therapeutic interventions. Through linkage mapping to chromosome 16 and high-throughput sequencing, mutations in a mitochondrial enzyme, glutamate pyruvate transaminase 2 (GPT2), have been identified in pedigrees affected by intellectual disability and postnatal microcephaly (Celis et al, 2015;Lobo-Prada et al, 2017;Ouyang et al, 2016). Also, a subset of patients has a progressive motor dysfunction, termed spastic paraplegia (Ouyang et al, 2016).…”

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confidence: 99%

The Role of Mitochondrial Glutamate Metabolism in Cognitive Development and Disease

Baytaş

Morrow

2017

Neuropsychopharmacol.

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Individual differences in the influence of task-irrelevant Pavlovian cues on human behavior. Front Behav Neurosci 9: 163. Kapur S (2003). Psychosis as a state of aberrant salience: a framework linking biology, phenomenology and pharmacology in schizophrenia. Am J Psychiatry 160: 13-23. Koshy Cherian A, Kucinski A, Pitchers K, YEgla B, Parikh V, Kim Y et al (2017). Unresponsive choline transporter as a trait neuromarker and a causal mediator of bottom-up attentional biases. J Neurosci 37: 2947-2959. Robinson TE, Yager LM, Cogan ES, Saunders BT (2014). On the motivational properties of reward cues: individual differences. Neuropharmacology 76(Part B): 450-459.

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A Homozygous Mutation in GPT2 Associated with Nonsyndromic Intellectual Disability in a Consanguineous Family from Costa Rica

Abstract: The mutation p. 96G>R c. 286G>A in GPT2, located in a loop where the substrate binds to the active site of the enzyme, fortifies the importance of GPT2 in the pathogenesis of nonsyndromic intellectual disability.

Cited by 6 publications

References 19 publications

Novel compound heterozygous mutations in GPT2 linked to microcephaly, and intellectual developmental disability with or without spastic paraplegia

Novel compound heterozygous mutations in GPT2 linked to microcephaly, and intellectual developmental disability with or without spastic paraplegia

GPT2 mutations cause developmental encephalopathy with microcephaly and features of complicated hereditary spastic paraplegia

The Role of Mitochondrial Glutamate Metabolism in Cognitive Development and Disease

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