1st Department of Obstetrics and Gynecology, Medical University of Warsaw, Pl. Starynkiewicza 1/3, 02-015, Warsaw, Poland.
Department of Medical Genetics, Medical University of Warsaw, ul Pawinskiego 3c, 02-106, Warsaw, Poland.
BMC Med Genet. 2019 Jul 31;20(1):132. doi: 10.1186/s12881-019-0865-0.
FOXL2 gene mutations cause blepharophimosis-ptosis-epicanthus inversus syndrome (BPES) and may be associated with premature ovarian insufficiency (POI). Two types of BPES were described in the literature. BPES type 2 is a simple association of inherited developmental defects of the eyelid area, while in type 1 female patients additionally suffer from POI. The following case study is the first report of endocrine impairments typical for menopausal transition in young female with NG_012454.1:g.138665342G > A, c.223C > T p.(Leu75Phe), mutation in FOXL2 gene. This mutation has been reported in the literature before, however until now, it was never linked to BPES type 1.
An 18-year-old nulliparous woman suspected of secondary amenorrhea was referred to our Endocrinology Outpatient Clinic. Blood tests revealed decreased levels of AMH (anti-Mullerian hormone) and increased levels of gonadotropins, suggesting menopausal transition. Her past medical history was remarkable for several ophthalmic defects that has required surgical interventions. BPES syndrome had not been suspected before, although the patient had reported a similar phenotype occurring in her father, sister and half-sister. Venous blood samples were collected from the female proband and from her three family members. Whole-exome sequencing and deep amplicon sequencing were performed. A potential pathogenic variant in the FOXL2 gene was revealed. Namely, the c.223C > T p.(Leu75Phe) missense variant was detected.
The authors found mutations, c.223C > T p.(Leu75Phe) in the FOXL2 gene in a young woman with hormonal disorders suggesting menopausal transition. These results indicate that the possibility of different phenotypes should be considered in patients with a similar genetic mutation.
FOXL2 基因突变导致睑裂狭小-上睑下垂-内眦赘皮倒向综合征(BPES),并可能与卵巢早衰(POI)有关。文献中描述了两种类型的 BPES。BPES 型 2 是眼睑区域遗传性发育缺陷的简单关联,而在 1 型女性患者中,还会出现 POI。以下病例研究是首例报告在携带 NG_012454.1:g.138665342G > A,c.223C > T p.(Leu75Phe),FOXL2 基因突变的年轻女性中出现绝经过渡的典型内分泌损伤。该突变以前在文献中已有报道,但直到现在,它从未与 1 型 BPES 相关联。
一位 18 岁的未婚女性因疑似继发性闭经被转至我们的内分泌门诊。血液检查显示 AMH(抗苗勒管激素)水平降低和促性腺激素水平升高,提示绝经过渡。她的既往病史有几个需要手术干预的眼科缺陷。以前没有怀疑过 BPES 综合征,尽管患者曾报告过她的父亲、姐姐和同父异母的妹妹也有类似的表型。从女性先证者和她的三位家庭成员中采集静脉血样本。进行了全外显子测序和深度扩增子测序。发现了 FOXL2 基因中的一个潜在致病变体。即,检测到 c.223C > T p.(Leu75Phe)错义变体。
作者在一名年轻女性中发现了 FOXL2 基因突变,c.223C > T p.(Leu75Phe),该女性有激素紊乱,提示绝经过渡。这些结果表明,对于具有类似遗传突变的患者,应考虑不同表型的可能性。
