Role of chromosomal imbalances in the pathogenesis of DSD: A retrospective analysis of 115 prenatal samples.

Mary, L; Fradin, M; Pasquier, L; Quelin, C; Loget, P; Le Lous, M; Le Bouar, G; Nivot-Adamiak, S; Lokchine, A; Dubourg, C; Jauffret, V; Nouyou, B; Henry, C; Launay, E; Odent, S; Jaillard, S; Belaud-Rotureau, M A

Mary, L; Fradin, M; Pasquier, L; Quelin, C; Loget, P; Le Lous, M; Le Bouar, G; Nivot-Adamiak, S; Lokchine, A; Dubourg, C; Jauffret, V; Nouyou, B; Henry, C; Launay, E; Odent, S; Jaillard, S; Belaud-Rotureau, M A.

Afiliação

Mary L; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France; Univ Rennes, CHU Rennes, Inserm, EHESP, Irset, UMR_S, 1085, F-35000, Rennes, France. Electronic address: laura.mary@chu-rennes.fr.
Fradin M; Service de Génétique Clinique, Centre de Référence Anomalies Du Développement, CLAD Ouest, CHU Rennes, Rennes, France.
Pasquier L; Service de Génétique Clinique, Centre de Référence Anomalies Du Développement, CLAD Ouest, CHU Rennes, Rennes, France; Université de Rennes, IGDR (Institut de Génétique et Développement), CNRS UMR 6290, INSERM ERL 1305, Rennes, France.
Quelin C; Service de Génétique Clinique, Centre de Référence Anomalies Du Développement, CLAD Ouest, CHU Rennes, Rennes, France.
Loget P; Service D'Anatomie Pathologique, Hôpital Pontchaillou, CHU Rennes, Rennes, France.
Le Lous M; Unité de Médecine FÅtale, Service de Gynécologie-Obstétrique, CHU Rennes, Rennes, France.
Le Bouar G; Unité de Médecine FÅtale, Service de Gynécologie-Obstétrique, CHU Rennes, Rennes, France.
Nivot-Adamiak S; Service D'endocrinologie Pédiatrique, CHU Rennes, Rennes, France.
Lokchine A; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France.
Dubourg C; Université de Rennes, IGDR (Institut de Génétique et Développement), CNRS UMR 6290, INSERM ERL 1305, Rennes, France; Service de Génétique Moléculaire et Génomique, CHU de Rennes, Rennes, 35033, France.
Jauffret V; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France.
Nouyou B; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France.
Henry C; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France.
Launay E; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France.
Odent S; Service de Génétique Clinique, Centre de Référence Anomalies Du Développement, CLAD Ouest, CHU Rennes, Rennes, France; Université de Rennes, IGDR (Institut de Génétique et Développement), CNRS UMR 6290, INSERM ERL 1305, Rennes, France.
Jaillard S; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France; Univ Rennes, CHU Rennes, Inserm, EHESP, Irset, UMR_S, 1085, F-35000, Rennes, France.
Belaud-Rotureau MA; CHU Rennes, Service de Cytogénétique et Biologie Cellulaire, F-35033, Rennes, France; Univ Rennes, CHU Rennes, Inserm, EHESP, Irset, UMR_S, 1085, F-35000, Rennes, France.

Eur J Med Genet ; 66(6): 104748, 2023 Jun.

Article em En | MEDLINE | ID: mdl-36948288

RESUMO

Differences of sex development (DSDs) are a group of congenital conditions characterized by a discrepancy between chromosomal, gonadal, and genital sex development of an individual, with significant impact on medical, psychological and reproductive life. The genetic heterogeneity of DSDs complicates the diagnosis and almost half of the patients remains undiagnosed. In this context, chromosomal imbalances in syndromic DSD patients may help to identify new genes implicated in DSDs. In this study, we aimed at describing the burden of chromosomal imbalances including submicroscopic ones (copy number variants or CNVs) in a cohort of prenatal syndromic DSD patients, and review their role in DSDs. Our patients carried at least one pathogenic or likely pathogenic chromosomal imbalance/CNV or low-level mosaicism for aneuploidy. Almost half of the cases resulted from an unbalanced chromosomal rearrangement. Chromosome 9p/q, 4p/q, 3q and 11q anomalies were more frequently observed. Review of the literature confirmed the causative role of CNVs in DSDs, either in disruption of known DSD-causing genes (SOX9, NR0B1, NR5A1, AR, ATRX, ) or as a tool to suspect new genes in DSDs (HOXD cluster, ADCY2, EMX2, CAMK1D, ). Recurrent CNVs of regulatory elements without coding sequence content (i.e. duplications/deletions upstream of SOX3 or SOX9) confirm detection of CNVs as a mean to explore our non-coding genome. Thus, CNV detection remains a powerful tool to explore undiagnosed DSDs, either through routine techniques or through emerging technologies such as long-read whole genome sequencing or optical genome mapping.

Assuntos

Aneuploidia; Translocação Genética; Gravidez; Feminino; Humanos; Estudos Retrospectivos; Mosaicismo; Variações do Número de Cópias de DNA; Cromossomos; Diagnóstico Pré-Natal/métodos

Palavras-chave

CMA; CNV; Chromosomal imbalance; DSD; Genital; Prenatal

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Translocação Genética / Aneuploidia Tipo de estudo: Diagnostic_studies / Etiology_studies / Observational_studies Limite: Female / Humans / Pregnancy Idioma: En Ano de publicação: 2023 Tipo de documento: Article

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