Gamma-aminobutyric acid transaminase (GABA-T) deficiency is an autosomal recessive disorder reported in only three unrelated families. It is caused by mutations in the ABAT gene, which encodes 4-aminobutyrate transaminase, an enzyme of GABA catabolism and mitochondrial nucleoside salvage. We report the case of a boy, deceased at 12 months of age, with early-onset epileptic encephalopathy, severe psychomotor retardation, hypotonia, lower-limb hyporeflexia, central hypoventilation, and rapid increase in weight and, to a lesser rate, length and head circumference. He presented signs of premature pubarche, thermal instability, and water-electrolyte imbalance. Serum total testosterone was elevated (43.3 ng/dl; normal range  T (p.Gln296His),not previously described. In vitro analysis concluded that this variant is pathogenic. The clinical features of this patient are similar to those reported so far in GABA-T deficiency. However, distinct mutations may have a different effect on enzymatic activity, which potentially could lead to a variable clinical outcome. Clinical investigation aiming for a diagnosis should not end with the patient's death, as it may allow a more precise genetic counselling for the family.info:eu-repo/semantics/publishedVersio

A Besse

A Pop

Alexandra Dinis

Ana Pop

Conceição Robalo

Cândida Cancelinha

Gajja S. Salomons

J Jaeken

Lina Ramos

LM Levy

Luísa Diogo

M Tsuji

MN Ritta

Olinda Rebelo

Paula Garcia

Pedro Louro

Raquel Pina

Ricardo Veiga

Louro, P

Ramos, L

Robalo, C

Cancelinha, C

Dinis, A

Veiga, R

Pina, R

Rebelo, O

Pop, A

Diogo, L

Salomons, GS

Garcia, P

CHUC Institutional Repository

Phenotyping GABA transaminase deficiency: a case description and literature review

Gamma‐aminobutyric acid transaminase (GABA‐T) deficiency is an autosomal recessive disorder reported in only three unrelated families. It is caused by mutations in the ABAT gene, which encodes 4‐aminobutyrate transaminase, an enzyme of GABA catabolism and mitochondrial nucleoside salvage. We report the case of a boy, deceased at 12 months of age, with early‐onset epileptic encephalopathy, severe psychomotor retardation, hypotonia, lower‐limb hyporeflexia, central hypoventilation, and rapid increase in weight and, to a lesser rate, length and head circumference. He presented signs of premature pubarche, thermal instability, and water–electrolyte imbalance. Serum total testosterone was elevated (43.3 ng/dl; normal range  T (p.Gln296His),not previously described. In vitro analysis concluded that this variant is pathogenic. The clinical features of this patient are similar to those reported so far in GABA‐T deficiency. However, distinct mutations may have a different effect on enzymatic activity, which potentially could lead to a variable clinical outcome. Clinical investigation aiming for a diagnosis should not end with the patient's death, as it may allow a more precise genetic counselling for the family

Louro, Pedro

Ramos, Lina

Robalo, Conceicao

Cancelinha, Candida

Dinis, Alexandra

Veiga, Ricardo

Pina, Raquel

Rebelo, Olinda

Pop, Ana

Diogo, Luisa

Salomons, Gajja S.

Garcia, Paula

NARCIS 

Gamma-aminobutyric acid transaminase (GABA-T) deficiency is an autosomal recessive disorder reported in only three unrelated families. It is caused by mutations in the ABAT gene, which encodes 4-aminobutyrate transaminase, an enzyme of GABA catabolism and mitochondrial nucleoside salvage. We report the case of a boy, deceased at 12 months of age, with early-onset epileptic encephalopathy, severe psychomotor retardation, hypotonia, lower-limb hyporeflexia, central hypoventilation, and rapid increase in weight and, to a lesser rate, length and head circumference. He presented signs of premature pubarche, thermal instability, and water-electrolyte imbalance. Serum total testosterone was elevated (43.3 ng/dl; normal range <16), as well as serum growth hormone (7.7 ng/ml; normal range <1). Brain magnetic resonance imaging (MRI) showed decreased myelination and generalized brain atrophy, later confirmed by post-mortem examination. ABAT gene sequencing was performed post-mortem, identifying a homozygous variant c.888G > T (p.Gln296His),not previously described. In vitro analysis concluded that this variant is pathogenic. The clinical features of this patient are similar to those reported so far in GABA-T deficiency. However, distinct mutations may have a different effect on enzymatic activity, which potentially could lead to a variable clinical outcome. Clinical investigation aiming for a diagnosis should not end with the patient's death, as it may allow a more precise genetic counselling for the family.info:eu-repo/semantics/publishedVersio

Name not available

Repositório Institucional dos Hospitais da Universidade de Coimbra

ORIGINAL ARTICLEPhenotyping GABA transaminase deficiency: a case descriptionand literature reviewPedro Louro1 & Lina Ramos1 & Conceição Robalo1 & Cândida Cancelinha1 &Alexandra Dinis1 & Ricardo Veiga1 & Raquel Pina1 & Olinda Rebelo1 & Ana Pop2 &Luísa Diogo1 & Gajja S. Salomons2 & Paula Garcia1Received: 19 April 2016 /Revised: 20 May 2016 /Accepted: 30 May 2016 /Published online: 4 July 2016# SSIEM 2016Abstract Gamma-aminobutyric acid transaminase (GABA-T) deficiency is an autosomal recessive disorder reported inonly three unrelated families. It is caused by mutations in theABAT gene, which encodes 4-aminobutyrate transaminase, anenzyme of GABA catabolism and mitochondrial nucleosidesalvage. We report the case of a boy, deceased at 12 months ofage, with early-onset epileptic encephalopathy, severe psycho-motor retardation, hypotonia, lower-limb hyporeflexia, centralhypoventilation, and rapid increase in weight and, to a lesserrate, length and head circumference. He presented signs ofpremature pubarche, thermal instability, and water–electrolyteimbalance. Serum total testosterone was elevated (43.3 ng/dl;normal range <16), as well as serum growth hormone(7.7 ng/ml; normal range <1). Brain magnetic resonance im-aging (MRI) showed decreased myelination and generalizedbrain atrophy, later confirmed by post-mortem examination.ABAT gene sequencing was performed post-mortem, identify-ing a homozygous variant c.888G > T (p.Gln296His),not pre-viously described. In vitro analysis concluded that this variantis pathogenic. The clinical features of this patient are similar tothose reported so far in GABA-T deficiency. However, dis-tinct mutations may have a different effect on enzymaticactivity, which potentially could lead to a variable clinicaloutcome. Clinical investigation aiming for a diagnosis shouldnot end with the patient’s death, as it may allow a more precisegenetic counselling for the family.Fig. 1 Patient’s photos (note the increasingly Bpuffy^ appearance) at2 months (a), 5 months (b), 10 months (c), and 11 months (d) of ageCommunicated by: Jaak Jaeken* Pedro Louropjplouro@gmail.com1 Centro Hospitalar e Universitário de Coimbra, Praceta Prof. MotaPinto, 3000-075 Coimbra, Portugal2 Metabolic Unit, Department of Clinical Chemistry, VU UniversityMedical Center, Neuroscience Campus Amsterdam,Amsterdam, The NetherlandsJ Inherit Metab Dis (2016) 39:743–747DOI 10.1007/s10545-016-9951-zFig. 2 Patient’s weight (a),length (b), and headcircumference growth (c) (growthcharts reproduced withpermission from World HealthOrganization)744 J Inherit Metab Dis (2016) 39:743–747IntroductionGamma-aminobutyric acid transaminase (GABA-T) deficien-cy (MIM#613163) is an autosomal recessive disorder reportedin only three unrelated families (Jaeken et al 1984; Tsuji et al2010; Besse et al 2015). It is caused by mutations in the ABATgene (HGNC_ID:23), which encodes 4-aminobutyrate trans-aminase (EC 2.6.1.19), an enzyme of GABA catabolism andmitochondrial nucleoside salvage (Besse et al 2015). GABA-T deficiency is usually characterized by elevated levels ofGABA in cerebrospinal fluid (CSF), associated with severepsychomotor retardation, intractable seizures, hypotonia withhyperreflexia, accelerated height growth, and a high-pitchedcry (Jaeken et al 1984; Tsuji et al 2010; Besse et al 2015).Case reportThe patient (Fig. 1) was a Portuguese male infant, born fullterm by caesarean delivery due to cephalopelvic dispropor-tion. He was the first child of healthy parents. Consanguinitywas denied but both parents originate from the samePortuguese region. He was admitted at the age of 3 days forgeneralized hypotonia since birth, progressing to encephalop-athy and coma. Electroencephalography (EEG) showed aburst-suppression pattern compatible with early-onset epilep-tic encephalopathy. Levetiracetam was started, initially reduc-ing the frequency of seizures, but ultimately with no effect.Until his death at the age of 12 months, he presented severepsychomotor retardation, lower-limb hyporeflexia, centralhypoventilation, bilateral cryptorchidism, and a rapid increasein weight, as well as in length and head circumference, al-though to a lesser rate (Fig. 2). He had a general “puffy”appearance, signs of premature pubarche, thermal instability,and water–electrolyte imbalance. He needed noninvasive ven-tilation and tube feeding.Serum total testosterone was elevated (43.3 ng/dl; normalrange <16), as was serum growth hormone (7.7 ng/ml; normalrange <1). Brain magnetic resonance imaging (MRI) showeddecreased myelination and generalized cerebral, cerebellar,and brainstem atrophy, later confirmed by post-mortem exam-ination. Diffusion-weighted images revealed bilateral hyper-intense areas involving subcortical and periventricular whitematter, and globus pallidus (Fig. 3). Magnetic resonance spec-troscopy (MRS) showed no abnormalities. Neuropathologicalexamination revealed soft consistency of the white matter.Microscopically, subcortical white matter is seen as a pale-stained/poorly myelinated area on the slide (Fig. 4).The diagnosis of GABA-T deficiencywas considered post-mortem. ABAT gene sequencing identified a homozygous var-iant c.888G > T (p.Gln296His), previously undescribed.MutationTaster, PolyPhen2 and SIFT predict this variant tobe, respectively, “disease causing”, “probably damaging”and “damaging”. In vitro analysis concluded that this variantis pathogenic (Pop et al 2015). At the time of the diagnosis, thepatient’s parents had an 11-weeks’ gestation. Chorionic villussampling was performed, and molecular analysis confirmedthat the fetus was not homozygous for the pathogenic variant.DiscussionThe clinical features of this patient are similar to those report-ed in GABA-T deficiency cases (Table 1). Interestingly,Fig. 3 Brain magnetic resonance imaging (MRI) at 12 months of age.Diffusion-weighted axial images show bilateral hyperintense areasinvolving subcortical and periventricular white matter, and globuspallidusFig. 4 Cerebral cortex and poorly myelinated subcortical white matter(Paraffin section, Klüver-Barrera staining, ×40) (a). Poorly myelinatedsubcortical white matter (Paraffin section, Klüver-Barrera staining,×200) (b)J Inherit Metab Dis (2016) 39:743–747 745Table1ClinicalfeaturesofreportedpatientsMainfeaturesPatient1aPatient2a(sibofpatient1)Patient3bPatient4cPatient5c(sibofpatient4)OurpatientMaleFemaleFemaleFemaleMaleMalePsychomotordelay++++++Refractoryseizures++++++Hypotonia++++++Hyperreflexia+++++-High-pitchedcry+++??+Adiposity++-??+Acceleratedlengthgrowth+++??+CT/MRIstructuralanomaliesGreatlyenlargedventricles,cisternae,andcorticalsulciGreatlyenlargedventricles,cisternae,andcorticalsulci-Generalizedcerebral,cerebellar,andbrainstematrophyGeneralizedatrophyoftherightcerebralhemisphereGeneralizedcerebral,cerebellar,andbrainstematrophySerumgrowthhormone(ng/ml)ND7.9-38.4(nl<5)8.84(nl0.28-1.64)??7.7(nl<1)CSFfreeGABA(μmol/L)ND4.8(nl0.04-0.12)1.26(nl0.04-0.12)??NDLymphoblastsGABA-T(pmol/h/mg)ND1.2(nl20-58)2(nl23-64)??NDGenotypedNDc.[659G>A];[1433T>C]c.[275G>A];[199-?_316+?del]c.[631C>T];[c.631C>T]c.[631C>T];[c.631C>T]c.[888G>T];[888G>T]DeducedeffectNDp.[Arg220Lys];[Leu478Pro]p.[Arg92Gln];[p.Asn67Valfs*8]p.[Leu211Phe];[p.Leu211Phe]p.[Leu211Phe];[p.Leu211Phe]p.[Gln296His];[Gln296His]Ageatdeath12months25monthsAliveat8yearsUnknown(aliveat5years)Aliveat5years12monthsPost-mortemexaminationofthebrainDilatedventriclesWhitematterwithasoftconsistencyPoormyelinationofgyralwhitematterSpongyleukodystrophyND?NDDilatedventriclesWhitematterwithasoftconsistencyGeneralizedleukodystrophyCTcomputedtomography,MRImagneticresonanceimaging,CSFcerebrospinalfluid,GABA-Tgamma-aminobutyricacidtransaminase,nlnormalrange,+present,−absent,NDnotdeterminedaJaekenetal.1984;bTsujietal.2010;cBesseetal.2015dReferencesequenceNM_000663.3746 J Inherit Metab Dis (2016) 39:743–747hyperreflexia was not present in our patient. His weight gainalmost overshadowed length growth. These growth alterationsseem to be related with the abnormally high levels of growthhormone, while the signs of premature pubarche are likely tobe related with the high testosterone levels, which may alsohave contributed to the patient’s “puffy” appearance. HighGABA levels probably contributed to this hormone imbalance(Jaeken et al 1990; Ritta et al 1998).Certain mutations express a residual enzymatic activity(Pop et al 2015), which potentially could lead to a variableclinical outcome. However, other (epi)genetic factors couldalso have an effect. CSF amino acid analysis was performedbut did not include free GABAmeasurement; when GABA-Tdeficiency was considered, it could not be performed due tothe lack of a CSF sample. This reinforces the need for therigorous implementation of sample collection and storing pro-tocols, mostly in severely affected patients, during life andeven at post-mortem. However, lumbar puncture is an inva-sive procedure, and sampling is not always easy. In our case,collected CSF volume was not enough to store.Detection of brain GABA elevation by MRS is difficultand usually requires a technical modification (Levy andDegnan 2013), which was not considered in this patient whilehe was alive. GABA-T is also involved in the mitochondrialnucleoside salvage pathway. Mitochondrial DNA (mtDNA)copy number measurement was not performed in our case,but an mtDNA depletion was previously demonstrated in fi-broblasts from other patients (Besse et al. 2015). Evidence of adepletion would probably have misled us to disorders withphenotypic overlap, such as the mtDNA depletion syndromescaused by mutations in SUCLG1 and SUCLA2 genes (Besseet al 2015). Clinical investigation aiming a diagnosis shouldnot end with the patient’s death, as it may allow a more precisegenetic counselling for the families. In our case, it allowed usto offer our patient’s parents a molecular prenatal diagnosis.Acknowledgments We thank Dr. Megumi Tsuji (Kanagawa Children'sMedical Centre, Japan) for her kind help.Compliance with ethical standardsConflict of interest None.ReferencesBesse A, Wu P, Bruni F, Donti T, Graham BH, Craigen WJ et al (2015)The GABA transaminase, ABAT, is essential for mitochondrial nu-cleoside metabolism. Cell Metab 21(3):417–427Jaeken J, Casaer P, de Cock P, Corbeel L, Eeckels R, Eggermont E et al(1984) Gamma-aminobutyric acid-transaminase deficiency: a newlyrecognized inborn error of neurotransmitter metabolism.Neuropediatrics 15(3):165–169Jaeken J, Casaer P, Haegele KD, Schechter PJ (1990) Review: normal andabnormal central nervous systemGABAmetabolism in childhood. JInherit Metab Dis 13(6):793–801Levy LM, Degnan AJ (2013) GABA-based evaluation of neurologicconditions: MR spectroscopy. Am J Neuroradiol 34(2):259–265Pop A, Janssen EAW, Roos B, Struys EA, Oostendorp J, Louro P et al(2015) Model system for fast in vitro analysis of GABA-T missensevariants [abstract]. J Inherit Metab Dis 38(Suppl 1):S315–S316Ritta MN, Calamera JC, Bas DE (1998) Occurrence of GABA andGABA receptors in human spermatozoa. Mol Hum Reprod 4(8):769–773Tsuji M, Aida N, Obata T, Tomiyasu M, Furuya N, Kurosawa K et al(2010) A new case of GABA transaminase deficiency facilitated byproton MR spectroscopy. J Inherit Metab Dis 33(1):85–90J Inherit Metab Dis (2016) 39:743–747 747

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Phenotyping GABA transaminase deficiency: a case description and literature review

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