Analysis of genetic variability in Turner syndrome linked to long-term clinical features

BACKGROUND: Women with Turner syndrome (TS) (45,X and related karyotypes) have an increased prevalence of conditions such as diabetes mellitus, obesity, hypothyroidism, autoimmunity, hypertension, and congenital cardiovascular anomalies (CCA). Whilst the risk of developing these co-morbidities may b...

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Autores principales: Suntharalingham, Jenifer P., Ishida, Miho, Cameron-Pimblett, Antoinette, McGlacken-Byrne, Sinead M., Buonocore, Federica, del Valle, Ignacio, Madhan, Gaganjit Kaur, Brooks, Tony, Conway, Gerard S., Achermann, John C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10548239/
https://www.ncbi.nlm.nih.gov/pubmed/37800145
http://dx.doi.org/10.3389/fendo.2023.1227164
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author Suntharalingham, Jenifer P.
Ishida, Miho
Cameron-Pimblett, Antoinette
McGlacken-Byrne, Sinead M.
Buonocore, Federica
del Valle, Ignacio
Madhan, Gaganjit Kaur
Brooks, Tony
Conway, Gerard S.
Achermann, John C.
author_facet Suntharalingham, Jenifer P.
Ishida, Miho
Cameron-Pimblett, Antoinette
McGlacken-Byrne, Sinead M.
Buonocore, Federica
del Valle, Ignacio
Madhan, Gaganjit Kaur
Brooks, Tony
Conway, Gerard S.
Achermann, John C.
author_sort Suntharalingham, Jenifer P.
collection PubMed
description BACKGROUND: Women with Turner syndrome (TS) (45,X and related karyotypes) have an increased prevalence of conditions such as diabetes mellitus, obesity, hypothyroidism, autoimmunity, hypertension, and congenital cardiovascular anomalies (CCA). Whilst the risk of developing these co-morbidities may be partly related to haploinsufficiency of key genes on the X chromosome, other mechanisms may be involved. Improving our understanding of underlying processes is important to develop personalized approaches to management. OBJECTIVE: We investigated whether: 1) global genetic variability differs in women with TS, which might contribute to co-morbidities; 2) common variants in X genes - on the background of haploinsufficiency - are associated with phenotype (a “two-hit” hypothesis); 3) the previously reported association of autosomal TIMP3 variants with CCA can be replicated. METHODS: Whole exome sequencing was undertaken in leukocyte DNA from 134 adult women with TS and compared to 46,XX controls (n=23), 46,XX women with primary ovarian insufficiency (n=101), and 46,XY controls (n=11). 1) Variability in autosomal and X chromosome genes was analyzed for all individuals; 2) the relation between common X chromosome variants and the long-term phenotypes listed above was investigated in a subgroup of women with monosomy X; 3) TIMP3 variance was investigated in relation to CCA. RESULTS: Standard filtering identified 6,457,085 autosomal variants and 126,335 X chromosome variants for the entire cohort, whereas a somatic variant pipeline identified 16,223 autosomal and 477 X chromosome changes. 1) Overall exome variability of autosomal genes was similar in women with TS and control/comparison groups, whereas X chromosome variants were proportionate to the complement of X chromosome material; 2) when adjusted for multiple comparisons, no X chromosome gene/variants were strongly enriched in monosomy X women with key phenotypes compared to monosomy X women without these conditions, although several variants of interest emerged; 3) an association between TIMP3 22:32857305:C-T and CCA was found (CCA 13.6%; non-CCA 3.4%, p<0.02). CONCLUSIONS: Women with TS do not have an excess of genetic variability in exome analysis. No obvious X-chromosome variants driving phenotype were found, but several possible genes/variants of interest emerged. A reported association between autosomal TIMP3 variance and congenital cardiac anomalies was replicated.
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spelling pubmed-105482392023-10-05 Analysis of genetic variability in Turner syndrome linked to long-term clinical features Suntharalingham, Jenifer P. Ishida, Miho Cameron-Pimblett, Antoinette McGlacken-Byrne, Sinead M. Buonocore, Federica del Valle, Ignacio Madhan, Gaganjit Kaur Brooks, Tony Conway, Gerard S. Achermann, John C. Front Endocrinol (Lausanne) Endocrinology BACKGROUND: Women with Turner syndrome (TS) (45,X and related karyotypes) have an increased prevalence of conditions such as diabetes mellitus, obesity, hypothyroidism, autoimmunity, hypertension, and congenital cardiovascular anomalies (CCA). Whilst the risk of developing these co-morbidities may be partly related to haploinsufficiency of key genes on the X chromosome, other mechanisms may be involved. Improving our understanding of underlying processes is important to develop personalized approaches to management. OBJECTIVE: We investigated whether: 1) global genetic variability differs in women with TS, which might contribute to co-morbidities; 2) common variants in X genes - on the background of haploinsufficiency - are associated with phenotype (a “two-hit” hypothesis); 3) the previously reported association of autosomal TIMP3 variants with CCA can be replicated. METHODS: Whole exome sequencing was undertaken in leukocyte DNA from 134 adult women with TS and compared to 46,XX controls (n=23), 46,XX women with primary ovarian insufficiency (n=101), and 46,XY controls (n=11). 1) Variability in autosomal and X chromosome genes was analyzed for all individuals; 2) the relation between common X chromosome variants and the long-term phenotypes listed above was investigated in a subgroup of women with monosomy X; 3) TIMP3 variance was investigated in relation to CCA. RESULTS: Standard filtering identified 6,457,085 autosomal variants and 126,335 X chromosome variants for the entire cohort, whereas a somatic variant pipeline identified 16,223 autosomal and 477 X chromosome changes. 1) Overall exome variability of autosomal genes was similar in women with TS and control/comparison groups, whereas X chromosome variants were proportionate to the complement of X chromosome material; 2) when adjusted for multiple comparisons, no X chromosome gene/variants were strongly enriched in monosomy X women with key phenotypes compared to monosomy X women without these conditions, although several variants of interest emerged; 3) an association between TIMP3 22:32857305:C-T and CCA was found (CCA 13.6%; non-CCA 3.4%, p<0.02). CONCLUSIONS: Women with TS do not have an excess of genetic variability in exome analysis. No obvious X-chromosome variants driving phenotype were found, but several possible genes/variants of interest emerged. A reported association between autosomal TIMP3 variance and congenital cardiac anomalies was replicated. Frontiers Media S.A. 2023-09-20 /pmc/articles/PMC10548239/ /pubmed/37800145 http://dx.doi.org/10.3389/fendo.2023.1227164 Text en Copyright © 2023 Suntharalingham, Ishida, Cameron-Pimblett, McGlacken-Byrne, Buonocore, del Valle, Madhan, Brooks, Conway and Achermann https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Suntharalingham, Jenifer P.
Ishida, Miho
Cameron-Pimblett, Antoinette
McGlacken-Byrne, Sinead M.
Buonocore, Federica
del Valle, Ignacio
Madhan, Gaganjit Kaur
Brooks, Tony
Conway, Gerard S.
Achermann, John C.
Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title_full Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title_fullStr Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title_full_unstemmed Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title_short Analysis of genetic variability in Turner syndrome linked to long-term clinical features
title_sort analysis of genetic variability in turner syndrome linked to long-term clinical features
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10548239/
https://www.ncbi.nlm.nih.gov/pubmed/37800145
http://dx.doi.org/10.3389/fendo.2023.1227164
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