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Revisiting GDF9 variants in primary ovarian insufficiency: A shift from dominant to recessive pathogenicity?
Jordan, Pénélope; Verebi, Camille; Hervé, Bérénice; Perol, Sandrine; Bernard, Valérie; Karila, Daphné; Jali, Eva; Brac de la Perrière, Aude; Grouthier, Virginie; Jonard-Catteau, Sophie; Touraine, Philippe; Fouveaut, Corinne; Plu-Bureau, Geneviève; Michel Dupont, Jean; Bachelot, Anne; Christin-Maitre, Sophie; Bienvenu, Thierry.
Affiliation
  • Jordan P; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France.
  • Verebi C; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France.
  • Hervé B; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France.
  • Perol S; Unité de gynécologie médicale, APHP. Centre Université Paris Cité, Hôpital Cochin Port-Royal, 75014 Paris, France.
  • Bernard V; Service de Chirurgie gynécologique et Médecine de la reproduction · Gynécologie médicale, CHU Bordeaux, Bordeaux, France.
  • Karila D; Service d'endocrinologie, diabétologie et médecine de la reproduction, APHP. Sorbonne Université, Hôpital Saint-Antoine, 75012 Paris, France.
  • Jali E; Service d'Endocrinologie, Hôpital de la Cavale Blanc, 29200 Brest, France.
  • Brac de la Perrière A; Service d'Endocrinologie, de diabétologie et des maladies métaboliques A, Hospices Civiles de Lyon, 69000 Lyon, France.
  • Grouthier V; Service d'Endocrinologie, Diabétologie et Nutrition, Hôpital Haut-Lévêque, CHU de Bordeaux, 33000 Bordeaux, France.
  • Jonard-Catteau S; Département d'assistance médicale à la procréation, Hôpital Jeanne de Flandre, 59000 Lille, France.
  • Touraine P; Département d'Endocrinologie et médecine de la reproduction, APHP. Sorbonne Université, Pitié-Salpêtrière Hospital, Center for Rare Endocrine and Gynecological Disorders, ERN-HCP, Paris, France.
  • Fouveaut C; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France.
  • Plu-Bureau G; Unité de gynécologie médicale, APHP. Centre Université Paris Cité, Hôpital Cochin Port-Royal, 75014 Paris, France.
  • Michel Dupont J; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France.
  • Bachelot A; Département d'Endocrinologie et médecine de la reproduction, APHP. Sorbonne Université, Pitié-Salpêtrière Hospital, Center for Rare Endocrine and Gynecological Disorders, ERN-HCP, Paris, France.
  • Christin-Maitre S; Service d'endocrinologie, diabétologie et médecine de la reproduction, APHP. Sorbonne Université, Hôpital Saint-Antoine, 75012 Paris, France.
  • Bienvenu T; Service de Médecine Génomique des Maladies de Système et d'Organe, Hôpital Cochin, APHP.Centre Université de Paris Cité, 75014 Paris, France. Electronic address: thierry.bienvenu@inserm.fr.
Gene ; 927: 148734, 2024 Nov 15.
Article in En | MEDLINE | ID: mdl-38942181
ABSTRACT

BACKGROUND:

Primary ovarian insufficiency (POI) affects around 2-4% of women before the age of 40. Genetic factors play an important role in POI. The GDF9 gene has been identified as a significant genetic contributor of POI. However, the pathogenicity and penetrance of GDF9 variants remain uncertain.

METHODS:

A next-generation sequencing approach was employed to investigate the entire coding region of the GDF9 gene in a cohort of 1281 patients with POI or diminished ovarian reserve (DOR). The frequency of each identified GDF9 variant was then compared with that of the general population, taking into account the ethnicity of each individual.

RESULTS:

By screening the entire coding region of the GDF9 gene, we identified 19 different variants, including 1 pathogenic frameshift variant. In total, 36 patients with POI/DOR (2.8%) carried at least one GDF9 variant. With regard to missense variants, no significant overrepresentation of the most common variants was observed in our POI/DOR cohort in comparison to the general or specific ethnic subgroups. Only one homozygous subject had a frameshift loss of function variant.

CONCLUSION:

This epidemiological study suggests that the vast majority of heterozygous missense variants could be considered as variants of uncertain significance and the homozygous loss-of-function variant could be considered as a pathogenic variant. The identification of a novel case of a homozygous POI patient with a heterozygous mother carrying the same variant with normal ovarian function strongly suggests that GDF9 syndrome is an autosomal recessive disorder.
Subject(s)
Key words

Full text: 1 Database: MEDLINE Main subject: Primary Ovarian Insufficiency / Growth Differentiation Factor 9 Limits: Adult / Female / Humans Language: En Journal: Gene Year: 2024 Type: Article Affiliation country: France

Full text: 1 Database: MEDLINE Main subject: Primary Ovarian Insufficiency / Growth Differentiation Factor 9 Limits: Adult / Female / Humans Language: En Journal: Gene Year: 2024 Type: Article Affiliation country: France