46,XY个体中类固醇生成因子-1的杂合突变可能模拟部分雄激素不敏感综合征。

Heterozygous mutation of steroidogenic factor-1 in 46,XY subjects may mimic partial androgen insensitivity syndrome.

作者信息

Coutant Régis, Mallet Delphine, Lahlou Najiba, Bouhours-Nouet Natacha, Guichet Agnès, Coupris Lionel, Croué Anne, Morel Yves

机构信息

Department of Pediatric Endocrinology, University Hospital, 4 rue Larrey, 49033 Angers Cedex 01, France.

出版信息

J Clin Endocrinol Metab. 2007 Aug;92(8):2868-73. doi: 10.1210/jc.2007-0024. Epub 2007 May 8.

DOI:10.1210/jc.2007-0024

PMID:17488792

Abstract

CONTEXT

The clinical and biological features of Sertoli cell and Leydig cell dysfunction are usually investigated when characterizing disorders of sex development in 46,XY individuals: This allows gonadal dysgenesis, a defective development of the gonad, to be distinguished from defects restricted to androgen synthesis or sensitivity. In humans, mutations in steroidogenic factor-1 (SF-1), one of the critical factors involved in testis development, have been reported to cause gonadal dysgenesis with or without adrenal failure in 46,XY individuals.

OBJECTIVE

We report a SF-1 mutation that caused ambiguous genitalia associated with strikingly different hormonal phenotypes in two affected 46,XY children from the same family.

METHODS

Hormonal evaluation included testosterone (T), anti-Mullerian hormone (AMH), inhibin B, FSH, and LH measurements during the first weeks of life, a period when physiological activation of the gonadotropin-gonadal system occurs. Direct DNA sequencing of the coding sequence of the SF-1 and the androgen receptor (AR) genes was performed.

RESULTS

Both 46,XY children had ambiguous genitalia with no Mullerian structures and no adrenal insufficiency. The older child showed normal elevation of T (up to 7.6 nmol/liter, 2.2 ng/ml), AMH (504 pmol/liter, 70.6 ng/ml), inhibin B (245 pg/ml), FSH, and LH during the first weeks, which led to a presumptive diagnosis of partial androgen insensitivity syndrome. The AR sequence was, however, normal. In the second child, T, AMH, and inhibin B were low, suggesting gonadal dysgenesis. In both children and their mother, a c.536delC frameshift mutation in the SF-1 gene was found. This mutation terminates translation at position 295, removing the ligand-binding domain and the activation function 2 (AF-2) domain, a critical domain for SF-1 transactivating activity.

CONCLUSIONS

The usual markers of testis dysgenesis may be normal in 46,XY individuals with SF-1 mutation. Screening for SF-1 mutation should be performed in subjects with apparent partial androgen insensitivity syndrome and no mutation in the AR gene.

摘要

背景

在对46,XY个体的性发育障碍进行特征描述时，通常会研究支持细胞和间质细胞功能障碍的临床及生物学特征：这有助于将性腺发育不全（性腺的缺陷性发育）与仅限于雄激素合成或敏感性的缺陷区分开来。在人类中，据报道，睾丸发育的关键因素之一类固醇生成因子-1（SF-1）的突变会导致46,XY个体出现有或无肾上腺功能不全的性腺发育不全。

目的

我们报告了一个SF-1突变，该突变在来自同一家族的两名受影响的46,XY儿童中导致了生殖器模糊，并伴有明显不同的激素表型。

方法

激素评估包括在生命的第一周内测量睾酮（T）、抗苗勒管激素（AMH）、抑制素B、促卵泡生成素（FSH）和促黄体生成素（LH），这是促性腺激素-性腺系统发生生理激活的时期。对SF-1和雄激素受体（AR）基因的编码序列进行直接DNA测序。

结果

两名46,XY儿童均有生殖器模糊，无苗勒管结构且无肾上腺功能不全。年龄较大的儿童在最初几周内T（高达7.6 nmol/L，2.2 ng/ml）、AMH（504 pmol/L，70.6 ng/ml）、抑制素B（245 pg/ml）、FSH和LH正常升高，这导致初步诊断为部分雄激素不敏感综合征。然而，AR序列正常。在第二个儿童中，T、AMH和抑制素B较低，提示性腺发育不全。在两名儿童及其母亲中，均发现SF-1基因存在c.536delC移码突变。该突变在第295位终止翻译，去除了配体结合结构域和激活功能2（AF-2）结构域，这是SF-1反式激活活性的关键结构域。