Prevalence and Changes in Genetic and Clinical Characteristics in Growth Hormone-Treated Belgian Girls with Turner Syndrome: A Study from the BELGROW Registry

Boutsen, Laure; Thomas, Muriel; De Schepper, Jean; Verlinde, Franciska; Beckers, Dominique; Heinrichs, Claudine; Vicinanza, Alfredo; Casteels, Kristina; Cools , Martine; Dotremont, Hilde; Brachet, Cecile; Parent, Anne-Simone; Chivu, Olimpia; MASSA, Guy; Klink, Daniel; Logghe, Karl; Depoorter, Sylvia; Fudvoye, Julie; Reynaert, Nele; Georis, Raphael; Becker, Marianne; Lysy, Philippe A.

Please use this identifier to cite or link to this item: http://hdl.handle.net/1942/48788

Title:	Prevalence and Changes in Genetic and Clinical Characteristics in Growth Hormone-Treated Belgian Girls with Turner Syndrome: A Study from the BELGROW Registry
Authors:	Boutsen, Laure Thomas, Muriel De Schepper, Jean Verlinde, Franciska Beckers, Dominique Heinrichs, Claudine Vicinanza, Alfredo Casteels, Kristina Cools , Martine Dotremont, Hilde Brachet, Cecile Parent, Anne-Simone Chivu, Olimpia MASSA, Guy Klink, Daniel Logghe, Karl Depoorter, Sylvia Fudvoye, Julie Reynaert, Nele Georis, Raphael Becker, Marianne Lysy, Philippe A.
Issue Date:	2026
Publisher:	KARGER
Source:	HORMONE RESEARCH IN PAEDIATRICS,
Status:	Early view
Abstract:	Introduction: Since the first description of Turner syndrome (TS), both genotypic spectrum and phenotypic presentation have evolved. This study aimed to examine trends in this evolution over the past three decades and provides an overview of current genetic and clinical features in a large nationwide multicenter cohort of girls with TS. Methods: We analyzed data from growth hormone (GH)-treated girls with TS included in BELGROW, the national GH registry of the BELux Society for Pediatric Endocrinology and Diabetology, between 1985 and 2022. Karyotype, age at diagnosis, and phenotype were studied in 716 girls. Two periods were compared: 1991-2002 (group 1, n = 250) and 2003-2017 (group 2, n = 270). Results: The annual number of girls with TS starting GH remained stable (mean n = 19/year). In the entire cohort, monosomy 45,X was the most frequent karyotype (44%), followed by structural anomalies of the X chromosome (27%), 45,X/46,XX mosaicism (13%), triple X mosaicism (4%), 45,X/46,XY or complex Y anomalies (6%), and others (6%). The proportion of 45,X decreased between the two periods (46%-38%, p < 0.05). Overall, median age at diagnosis was 6.4 years with 7.6% of girls diagnosed prenatally, 24% before age 1, 49% in childhood, and 19% after 12 years. Prenatal diagnoses increased from 2.5% (group 1) to 15% (group 2) (p < 0.001). Girls with a 45,X karyotype were diagnosed earlier than girls with other genotypes (median 2.2 vs. 8 years, p < 0.001). Skeletal (73%), neurosensory (60%), and cardiac (29%) systems were most affected. Skeletal and cardiac malformations were more frequent in girls with a 45,X karyotype (p < 0.05 and p < 0.01, respectively). Conclusion: Genotype distribution and timing of TS diagnosis have significantly changed since 1991, while the annual number of girls starting GH therapy has remained stable. A 45,X karyotype is associated with earlier diagnosis and more comorbidities.
Notes:	Lysy, PA (corresponding author), Clin Univ St Luc, Serv Specialized Pediat, Pediat Endocrinol Unit, Brussels, Belgium.; Lysy, PA (corresponding author), BElgian & Luxembourgish Soc Pediat Endocrinol & Di, Brussels, Belgium. philippe.lysy@saintluc.uclouvain.be
Keywords:	Turner syndrome;Growth hormone;Genotype;Phenotype;BELGROW
Document URI:	http://hdl.handle.net/1942/48788
DOI:	10.1159/000550509
ISI #:	001712412500001
Rights:	2026 S. Karger AG, Basel
Category:	A1
Type:	Journal Contribution
Appears in Collections:	Research publications

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