Author:
Bachelot Anne,Rouxel Agnès,Massin Nathalie,Dulon Jérome,Courtillot Carine,Matuchansky Christine,Badachi Yasmina,Fortin Anne,Paniel Bernard,Lecuru Fabrice,Lefrère-Belda Marie-Aude,Constancis Elisabeth,Thibault Elisabeth,Meduri Géri,Guiochon-Mantel Anne,Misrahi Micheline,Kuttenn Frédérique,Touraine Philippe,_ _
Abstract
ObjectivePremature ovarian failure (POF) encompasses a heterogeneous spectrum of conditions, with phenotypic variability among patients. The etiology of POF remains unknown in most cases. We performed a global phenotyping of POF women with the aim of better orienting attempts at an etiological diagnosis.Design and methodsWe performed a mixed retrospective and prospective study of clinical, biological, histological, morphological, and genetic data relating to 357 consecutive POF patients between 1997 and 2008. The study was conducted at a reproductive endocrinology referral center.ResultsSeventy-six percent of the patients presented with normal puberty and secondary amenorrhea. Family history was present in 14% of the patients, clinical and/or biological autoimmunity in 14.3%. Fifty-six women had a fluctuating form of POF. The presence of follicles was suggested at ultrasonography in 50% of the patients, and observed in 29% at histology; the negative predictive value of the presence of follicles at ultrasonography was 77%. Bone mineral density alterations were found in 58% of the women. Eight patients had X chromosomal abnormalities other than Turner's syndrome, eight other patients evidenced FMR1 pre-mutation. Two other patients had autoimmune polyendocrine syndrome type 2 and 1.ConclusionA genetic cause of POF was identified in 25 patients, i.e. 7% of the whole cohort. POF etiology remains most often undiscovered. Novel strategies of POF phenotyping are in such content mandatory to improve the rate of POF patients for whom etiology is identified.
Subject
Endocrinology,General Medicine,Endocrinology, Diabetes and Metabolism
Cited by
115 articles.
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