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抗苗勒管激素表明脆性X智力低下(FMR1)前突变携带者存在早期卵巢功能衰退:一项初步研究。

Anti-Mullerian hormone indicates early ovarian decline in fragile X mental retardation (FMR1) premutation carriers: a preliminary study.

作者信息

Rohr J, Allen E G, Charen K, Giles J, He W, Dominguez C, Sherman S L

机构信息

Department of Human Genetics, Emory University School of Medicine, 615 Michael Street, Suite 301, Whitehead Building, Atlanta, GA 30322, USA.

出版信息

Hum Reprod. 2008 May;23(5):1220-5. doi: 10.1093/humrep/den050. Epub 2008 Mar 1.

DOI:10.1093/humrep/den050
PMID:18310677
Abstract

BACKGROUND

Women who carry the fragile X mental retardation (FMR1) premutation are at risk for fragile X-associated primary ovarian insufficiency. Past studies have shown that carriers who are still cycling have increased levels FSH compared with non-carriers. As anti-Mullerian hormone (AMH) has been shown as an excellent marker of ovarian decline, we examined AMH levels among premutation carriers to characterize their ovarian function.

METHODS

We determined the level of FSH and AMH in serum samples collected during early follicular phase from women who carried longer FMR1 repeat alleles (defined as >or=70 repeats, n = 40) and those with shorter repeat alleles (<70 repeats, n = 75), identified by DNA analysis. Comparisons were made stratified by age and carrier status.

RESULTS

For all age groups, AMH levels were significantly lower among longer repeat allele carriers compared to shorter repeat allele carriers (P = 0.002, 0.006 and 0.020 for women ages 18-30, 31-40 and 41-50 years, respectively). In contrast, increased FSH indicative of early ovarian decline was only evident for longer repeat allele carriers aged 31-40 years (P = 0.089, 0.001 and 0.261 for women ages 18-30, 31-40 and 41-50 years, respectively).

CONCLUSIONS

These preliminary data suggest that AMH levels indicate early ovarian decline among women with longer FMR1 repeat alleles; moreover, AMH appears to be a better marker than FSH in identifying this early decline.

摘要

背景

携带脆性X智力低下1(FMR1)前突变的女性有患脆性X相关原发性卵巢功能不全的风险。既往研究表明,仍有月经周期的携带者与非携带者相比,促卵泡生成素(FSH)水平升高。由于抗苗勒管激素(AMH)已被证明是卵巢功能衰退的良好标志物,我们检测了前突变携带者的AMH水平以表征其卵巢功能。

方法

我们通过DNA分析确定了携带较长FMR1重复等位基因(定义为≥70次重复,n = 40)和较短重复等位基因(<70次重复,n = 75)的女性在卵泡早期采集的血清样本中FSH和AMH的水平。按年龄和携带者状态进行分层比较。

结果

在所有年龄组中,较长重复等位基因携带者的AMH水平显著低于较短重复等位基因携带者(18 - 30岁、31 - 40岁和41 - 50岁女性的P值分别为0.002、0.006和0.020)。相比之下,提示卵巢功能早期衰退的FSH升高仅在31 - 40岁的较长重复等位基因携带者中明显(18 - 30岁、31 - 40岁和41 - 50岁女性的P值分别为0.089、0.001和0.261)。

结论

这些初步数据表明,AMH水平提示携带较长FMR1重复等位基因女性的卵巢功能早期衰退;此外,在识别这种早期衰退方面,AMH似乎是比FSH更好的标志物。

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