Novel likely pathogenic variants in TMEM126A identified in non-syndromic autosomal recessive optic atrophy: two case reports

Katja Kloth; Matthis Synofzik; Christoph Kernstock; Simone Schimpf-Linzenbold; Frank Schuettauf; Axel Neu; Bernd Wissinger; Nicole Weisschuh

doi:10.1186/s12881-019-0795-x

BMC Medical Genetics (Apr 2019)

Novel likely pathogenic variants in TMEM126A identified in non-syndromic autosomal recessive optic atrophy: two case reports

Katja Kloth,
Matthis Synofzik,
Christoph Kernstock,
Simone Schimpf-Linzenbold,
Frank Schuettauf,
Axel Neu,
Bernd Wissinger,
Nicole Weisschuh

Affiliations

Katja Kloth: Institute of Human Genetics, University Medical Center Hamburg-Eppendorf
Matthis Synofzik: Department of Neurodegenerative Diseases, Hertie Institute for Clinical Brain Research, University of Tübingen
Christoph Kernstock: Center for Ophthalmology, Institute for Ophthalmic Research, University of Tübingen
Simone Schimpf-Linzenbold: CeGaT GmbH and Praxis für Humangenetik Tübingen
Frank Schuettauf: Department of Ophthalmology, University Medical Center Hamburg-Eppendorf
Axel Neu: Department of Pediatrics, University Medical Center Hamburg-Eppendorf
Bernd Wissinger: Center for Ophthalmology, Institute for Ophthalmic Research, University of Tübingen
Nicole Weisschuh: Center for Ophthalmology, Institute for Ophthalmic Research, University of Tübingen

DOI: https://doi.org/10.1186/s12881-019-0795-x
Journal volume & issue: Vol. 20, no. 1
pp. 1 – 10

Abstract

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Abstract Background Reports on autosomal recessive optic atrophy (arOA) are sparse and so far, only one gene has been specifically associated with non-syndromic arOA, namely TMEM126A. To date, all reports of pathogenic TMEM126A variants are from affected individuals of Maghrebian origin, who all carry an identical nonsense variant. Here we report two novel variants in the TMEM126A gene from non-Maghreb individuals, both found in affected individuals with an arOA phenotype. Case presentation We report three affected individuals from two families. The proband of family A, a 24-year-old Turkish woman, was diagnosed with visual loss in early childhood but a diagnosis of optic atrophy was only made at 14 years. A diagnostic gene panel revealed a splice donor variant (c.86 + 2 T > C) in homozygous state in the TMEM126A gene. Analysis of this variant based on RNA from whole blood revealed a single aberrant transcript lacking exon 2, presumably representing a functional null allele. Two siblings from family B, a 16-year old Iraqi girl and her 14-year old brother, were diagnosed with optic atrophy in early childhood. A missense variant p.(S36 L) in the TMEM126A gene was identified in homozygous state in a gene panel-based diagnostic setting in both siblings. This missense variant is ultra rare in the general population, affects a highly evolutionarily conserved amino acid and segregates with the disease within the family. The three probands reported in this study had a relatively mild clinical course without any evidence of a syndromic (e.g. neurological) comorbidity, which is in line with previous studies. Conclusions We provide additional evidence for the implication of biallelic pathogenic TMEM126A variants in arOA. Our findings extend both the mutational spectrum and geographic presence of TMEM126A in arOA. Screening of the entire gene should be considered in affected individuals presenting with features resembling arOA and also from non-Maghrebian descent.

Published in BMC Medical Genetics

ISSN: 1471-2350 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenet.biomedcentral.com

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