The matter of significance – Has the p.(Glu121Lys) variant of TOR1A gene a pathogenic role in dystonia or Parkinson disease?

The matter of significance – Has the p.(Glu121Lys) variant of TOR1A gene a pathogenic role in dystonia or Parkinson disease?

•Whole exome sequencing become powerful tool in new pathogenic variants identification.•The TOR1A p.Glu121Lys is not pathogenic variant.•Genetic databeses should be updated based on the analysis on well characterized cohorts. Next Generation Sequencing (NGS), has now become a very powerful tool for...

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Veröffentlicht in:Journal of clinical neuroscience 2020-02, Vol.72, p.501-503
Hauptverfasser: Milanowski, Łukasz, Hoffman-Zacharska, Dorota, Geremek, Maciej, Friedman, Andrzej, Figura, Monika, Koziorowski, Dariusz
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Sprache:eng
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Differential diagnosis
Parkinson disease
Primary dystonia
TOR1A
WES
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container_start_page 501
container_title Journal of clinical neuroscience
container_volume 72
creator Milanowski, Łukasz
Hoffman-Zacharska, Dorota
Geremek, Maciej
Friedman, Andrzej
Figura, Monika
Koziorowski, Dariusz
description •Whole exome sequencing become powerful tool in new pathogenic variants identification.•The TOR1A p.Glu121Lys is not pathogenic variant.•Genetic databeses should be updated based on the analysis on well characterized cohorts. Next Generation Sequencing (NGS), has now become a very powerful tool for decoding variants of genes involved in pathogenesis of number of human disorders. One of the challenges of this method is to decipher the real pathogenic variants from a number of identified, not related to the disorder in analyzed case. Another issue is recognition of new phenotypes previously unrecognized but related to new variants combinations’ in known genes. The other aspect is the HGMD or ClinVar mutation databases usage in data interpretation. The aim of this paper is to discuss pathogenicity of p.(Glu121Lys) missense mutation in the TOR1A gene previously described as dystonia causing variant. The patient diagnosed with typical Parkinson disease and positive family history was included into analysis. Also the internal whole exome sequencing (WES) database containing 600 subjects who has performed WES due to different causes was searched. All subjects had WES performed on SureSelect Human All Exon v.6 enrichment, Illumina NovaSeq 6000 platform, (annotations according to internal Institute Mother and Child’s pipeline). The TOR1A p.(Glu121Lys) heterozygous mutation was revealed in 1 patient diagnosed with PD and 2 healthy subjects who has no dystonia symptoms. To conclude the TOR1A p.Glu121Lys variant should not be recognized as clearly pathogenic now.
doi_str_mv 10.1016/j.jocn.2019.12.018
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source Elsevier ScienceDirect Journals
subjects Differential diagnosis
Parkinson disease
Primary dystonia
TOR1A
WES
title The matter of significance – Has the p.(Glu121Lys) variant of TOR1A gene a pathogenic role in dystonia or Parkinson disease?
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