par Rosenthal, Ira I.M.;Refetoff, Samuel 
;Rich, Barry;Barnes, Randall R.B.;Sunthornthepvarakul, Thongkum;Parma, Jasmine ;Rosenfield, Robert R.L.
Référence The Journal of clinical endocrinology and metabolism, 81, 10, page (3802-3806)
Publication Publié, 1996
;Rich, Barry;Barnes, Randall R.B.;Sunthornthepvarakul, Thongkum;Parma, Jasmine ;Rosenfield, Robert R.L.Référence The Journal of clinical endocrinology and metabolism, 81, 10, page (3802-3806)
Publication Publié, 1996
Article révisé par les pairs
| Résumé : | The pituitary-gonadal axis was evaluated in a mother after two of her sons with familial male-limited pseudoprecocious puberty were found to have a constitutively activating mutation of the LH receptor (LHR). Genotyping demonstrated that all showed a mutation in one of the two alleles, a substitution of Gly for Asp578 in the sixth transmembrane segment of the LHR. Ovarian function was normal in the 36-yr-old mother as assessed by LH dynamics and FSH and androgen levels throughout the menstrual cycle. Hormonal responses to acute GnRH agonist (nafarelin) challenge, chronic GnRH agonist administration, and dexamethasone were also normal. Studies of the boys upon presentation at 2.4 and 3.5 yr of age revealed that acute LH responses to nafarelin were in the hypogonadotropic range, and the FSH responses were prepubertal despite the presence of late pubertal testosterone blood levels. Upon the inception of true puberty at 11 yr of age in the older brother, gonadotropin responses normalized for the state of development. The data show that this activating LHR mutation does not cause functional ovarian hyperandrogenism and causes only incomplete pubertal activation of Leydig cells. The results are compatible with relatively low constitutive activity associated with this structural abnormality of LHR. |
