Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank

Deletions spanning the STS (steroid sulfatase) gene at Xp22.31 are associated with X-linked ichthyosis, corneal opacities, testicular maldescent, cardiac arrhythmia, and higher rates of developmental and mood disorders/traits, possibly related to the smaller volume of some basal ganglia structures....

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Autores principales: Gubb, Samuel J A, Brcic, Lucija, Underwood, Jack F G, Kendall, Kimberley M, Caseras, Xavier, Kirov, George, Davies, William
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2020
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General Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7566349/
https://www.ncbi.nlm.nih.gov/pubmed/32766777
http://dx.doi.org/10.1093/hmg/ddaa174
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author Gubb, Samuel J A
Brcic, Lucija
Underwood, Jack F G
Kendall, Kimberley M
Caseras, Xavier
Kirov, George
Davies, William
author_facet Gubb, Samuel J A
Brcic, Lucija
Underwood, Jack F G
Kendall, Kimberley M
Caseras, Xavier
Kirov, George
Davies, William
author_sort Gubb, Samuel J A
collection PubMed
description Deletions spanning the STS (steroid sulfatase) gene at Xp22.31 are associated with X-linked ichthyosis, corneal opacities, testicular maldescent, cardiac arrhythmia, and higher rates of developmental and mood disorders/traits, possibly related to the smaller volume of some basal ganglia structures. The consequences of duplication of the same genomic region have not been systematically assessed in large or adult samples, although evidence from case reports/series has indicated high rates of developmental phenotypes. We compared multiple measures of physical and mental health, cognition and neuroanatomy in male (n = 414) and female (n = 938) carriers of 0.8–2.5 Mb duplications spanning STS, and non-carrier male (n = 192, 826) and female (n = 227, 235) controls from the UK Biobank (recruited aged 40–69 from the UK general population). Clinical and self-reported diagnoses indicated a higher prevalence of inguinal hernia and mania/bipolar disorder respectively in male duplication carriers, and a higher prevalence of gastro-oesophageal reflux disease and blistering/desquamating skin disorder respectively in female duplication carriers; duplication carriers also exhibited reductions in several depression-related measures, and greater happiness. Cognitive function and academic achievement did not differ between comparison groups. Neuroanatomical analysis suggested greater lateral ventricle and putamen volume in duplication carriers. In conclusion, Xp22.31 duplications appear largely benign, but could slightly increase the likelihood of specific phenotypes (although results were only nominally-significant). In contrast to deletions, duplications might protect against depressive symptoms, possibly via higher STS expression/activity (resulting in elevated endogenous free steroid levels), and through contributing towards an enlarged putamen volume. These results should enable better genetic counselling of individuals with Xp22.31 microduplications.
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spelling pubmed-75663492020-10-21 Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank Gubb, Samuel J A Brcic, Lucija Underwood, Jack F G Kendall, Kimberley M Caseras, Xavier Kirov, George Davies, William Hum Mol Genet General Article Deletions spanning the STS (steroid sulfatase) gene at Xp22.31 are associated with X-linked ichthyosis, corneal opacities, testicular maldescent, cardiac arrhythmia, and higher rates of developmental and mood disorders/traits, possibly related to the smaller volume of some basal ganglia structures. The consequences of duplication of the same genomic region have not been systematically assessed in large or adult samples, although evidence from case reports/series has indicated high rates of developmental phenotypes. We compared multiple measures of physical and mental health, cognition and neuroanatomy in male (n = 414) and female (n = 938) carriers of 0.8–2.5 Mb duplications spanning STS, and non-carrier male (n = 192, 826) and female (n = 227, 235) controls from the UK Biobank (recruited aged 40–69 from the UK general population). Clinical and self-reported diagnoses indicated a higher prevalence of inguinal hernia and mania/bipolar disorder respectively in male duplication carriers, and a higher prevalence of gastro-oesophageal reflux disease and blistering/desquamating skin disorder respectively in female duplication carriers; duplication carriers also exhibited reductions in several depression-related measures, and greater happiness. Cognitive function and academic achievement did not differ between comparison groups. Neuroanatomical analysis suggested greater lateral ventricle and putamen volume in duplication carriers. In conclusion, Xp22.31 duplications appear largely benign, but could slightly increase the likelihood of specific phenotypes (although results were only nominally-significant). In contrast to deletions, duplications might protect against depressive symptoms, possibly via higher STS expression/activity (resulting in elevated endogenous free steroid levels), and through contributing towards an enlarged putamen volume. These results should enable better genetic counselling of individuals with Xp22.31 microduplications. Oxford University Press 2020-08-07 /pmc/articles/PMC7566349/ /pubmed/32766777 http://dx.doi.org/10.1093/hmg/ddaa174 Text en © The Author(s) 2020. Published by Oxford University Press. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle General Article
Gubb, Samuel J A
Brcic, Lucija
Underwood, Jack F G
Kendall, Kimberley M
Caseras, Xavier
Kirov, George
Davies, William
Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title_full Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title_fullStr Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title_full_unstemmed Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title_short Medical and neurobehavioural phenotypes in male and female carriers of Xp22.31 duplications in the UK Biobank
title_sort medical and neurobehavioural phenotypes in male and female carriers of xp22.31 duplications in the uk biobank
topic General Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7566349/
https://www.ncbi.nlm.nih.gov/pubmed/32766777
http://dx.doi.org/10.1093/hmg/ddaa174
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