TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels

Ewout Muylle; Huafang Jiang; Christin Johnsen; Seul Kee Byeon; Wasantha Ranatunga; Kishore Garapati; Roman M. Zenka; Graeme Preston; Akhilesh Pandey; Tamas Kozicz; Fang Fang; Eva Morava

doi:10.1002/jimd.12550

TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels

Ewout Muylle, Huafang Jiang, Christin Johnsen, Seul Kee Byeon, Wasantha Ranatunga, Kishore Garapati, Roman M. Zenka, Graeme Preston, Akhilesh Pandey, Tamas Kozicz, Fang Fang, Eva Morava

Research output: Contribution to journal › Review article › peer-review

Abstract

TRIT1 defect is a rare, autosomal-recessive disorder of transcription, initially described as a condition with developmental delay, myoclonic seizures, and abnormal mitochondrial function. Currently, only 13 patients have been reported. We reviewed the genetic, clinical, and metabolic aspects of the disease in all known patients, including two novel, unrelated TRIT1 cases with abnormalities in oxidative phosphorylation complexes I and IV in fibroblasts. Taken together the features of all 15 patients, TRIT1 defect could be identified as a potentially recognizable syndrome including myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and variable microcephaly, with normal lactate levels. Half of the patients had oxidative phosphorylation complex measurements and had multiple complex abnormalities.

Original language	English (US)
Pages (from-to)	1039-1047
Number of pages	9
Journal	Journal of inherited metabolic disease
Volume	45
Issue number	6
DOIs	https://doi.org/10.1002/jimd.12550
State	Published - Nov 2022

Keywords

OXPHOS
lipidomics
mitochondrial tRNA
myoclonic seizures
spasticity

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1002/jimd.12550

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Muylle, E., Jiang, H., Johnsen, C., Byeon, S. K., Ranatunga, W., Garapati, K., Zenka, R. M., Preston, G., Pandey, A., Kozicz, T., Fang, F., & Morava, E. (2022). TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels. Journal of inherited metabolic disease, 45(6), 1039-1047. https://doi.org/10.1002/jimd.12550

Muylle, E, Jiang, H, Johnsen, C, Byeon, SK, Ranatunga, W, Garapati, K, Zenka, RM, Preston, G, Pandey, A , Kozicz, T, Fang, F & Morava, E 2022, 'TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels', Journal of inherited metabolic disease, vol. 45, no. 6, pp. 1039-1047. https://doi.org/10.1002/jimd.12550

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title = "TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels",

abstract = "TRIT1 defect is a rare, autosomal-recessive disorder of transcription, initially described as a condition with developmental delay, myoclonic seizures, and abnormal mitochondrial function. Currently, only 13 patients have been reported. We reviewed the genetic, clinical, and metabolic aspects of the disease in all known patients, including two novel, unrelated TRIT1 cases with abnormalities in oxidative phosphorylation complexes I and IV in fibroblasts. Taken together the features of all 15 patients, TRIT1 defect could be identified as a potentially recognizable syndrome including myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and variable microcephaly, with normal lactate levels. Half of the patients had oxidative phosphorylation complex measurements and had multiple complex abnormalities.",

keywords = "OXPHOS, lipidomics, mitochondrial tRNA, myoclonic seizures, spasticity",

author = "Ewout Muylle and Huafang Jiang and Christin Johnsen and Byeon, {Seul Kee} and Wasantha Ranatunga and Kishore Garapati and Zenka, {Roman M.} and Graeme Preston and Akhilesh Pandey and Tamas Kozicz and Fang Fang and Eva Morava",

note = "Publisher Copyright: {\textcopyright} 2022 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM.",

year = "2022",

month = nov,

doi = "10.1002/jimd.12550",

language = "English (US)",

volume = "45",

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AU - Muylle, Ewout

AU - Jiang, Huafang

AU - Johnsen, Christin

AU - Byeon, Seul Kee

AU - Ranatunga, Wasantha

AU - Garapati, Kishore

AU - Zenka, Roman M.

AU - Preston, Graeme

AU - Pandey, Akhilesh

AU - Kozicz, Tamas

AU - Fang, Fang

AU - Morava, Eva

PY - 2022/11

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N2 - TRIT1 defect is a rare, autosomal-recessive disorder of transcription, initially described as a condition with developmental delay, myoclonic seizures, and abnormal mitochondrial function. Currently, only 13 patients have been reported. We reviewed the genetic, clinical, and metabolic aspects of the disease in all known patients, including two novel, unrelated TRIT1 cases with abnormalities in oxidative phosphorylation complexes I and IV in fibroblasts. Taken together the features of all 15 patients, TRIT1 defect could be identified as a potentially recognizable syndrome including myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and variable microcephaly, with normal lactate levels. Half of the patients had oxidative phosphorylation complex measurements and had multiple complex abnormalities.

AB - TRIT1 defect is a rare, autosomal-recessive disorder of transcription, initially described as a condition with developmental delay, myoclonic seizures, and abnormal mitochondrial function. Currently, only 13 patients have been reported. We reviewed the genetic, clinical, and metabolic aspects of the disease in all known patients, including two novel, unrelated TRIT1 cases with abnormalities in oxidative phosphorylation complexes I and IV in fibroblasts. Taken together the features of all 15 patients, TRIT1 defect could be identified as a potentially recognizable syndrome including myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and variable microcephaly, with normal lactate levels. Half of the patients had oxidative phosphorylation complex measurements and had multiple complex abnormalities.

KW - OXPHOS

KW - lipidomics

KW - mitochondrial tRNA

KW - myoclonic seizures

KW - spasticity

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TRIT1 defect leads to a recognizable phenotype of myoclonic epilepsy, speech delay, strabismus, progressive spasticity, and normal lactate levels

Abstract

Keywords

ASJC Scopus subject areas

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