Chouchene Ibtissem, Derouiche Kaouthar, Chaabouni Afif, Cherif Lamia, Amouri Ahlem, Largueche Leila, Abdelhak Sonia, El Matri Leila
Genet Test Mol Biomarkers. 2010 Feb;14(1):145-8. doi: 10.1089/gtmb.2009.0091.
Mutations in FOXL2 gene are responsible for blepharophimosis ptosis epicanthus inversus and telecanthus syndrome (BPES). The BPES syndrome is a rare autosomal dominant genetic disease characterized by eyelid malformations associated with premature ovarian failure (BPES type I) or not (BPES type II). The human FOXL2 protein (376 aa) contains a 100 amino-acid DNA-binding forkhead domain (residues 52-152) and a polyalanine tract (residues 221-234). In the present study, we report the molecular investigation of four affected members with BPES syndrome in a Tunisian consanguineous family. To identify the causative mutation, we performed a direct sequencing of the FOXL2 gene. The sequence analysis of the coding exon revealed a novel frameshift mutation g.1113 dup C, c.876 dup C, p.P292 Fs. The mutation is located downstream of the polyalanine tract and causes the protein extension to 532 aa. This study reports for the first time a novel frameshift mutation in two-generation consanguineous Tunisian family with BPES. Our results expand the spectrum of FOXL2 mutations.
FOXL2基因突变是睑裂狭小-上睑下垂-内眦赘皮-睑裂增宽综合征(BPES)的病因。BPES综合征是一种罕见的常染色体显性遗传病,其特征为眼睑畸形,伴有(BPES I型)或不伴有(BPES II型)卵巢早衰。人类FOXL2蛋白(376个氨基酸)包含一个100个氨基酸的DNA结合叉头结构域(第52至152位氨基酸)和一个聚丙氨酸束(第221至234位氨基酸)。在本研究中,我们报告了对一个突尼斯近亲家庭中四名BPES综合征患者的分子研究。为了鉴定致病突变,我们对FOXL2基因进行了直接测序。编码外显子的序列分析揭示了一个新的移码突变g.1113 dup C、c.876 dup C、p.P292 Fs。该突变位于聚丙氨酸束下游,导致蛋白质延伸至532个氨基酸。本研究首次报道了一个突尼斯近亲两代家庭中BPES的新移码突变。我们的结果扩展了FOXL2突变谱。
