雷特综合征
遗传学
生物
单倍率不足
MECP2
点突变
突变
外显子
表型
基因
作者
Christophe Philippe,Daniel Amsallem,Christine Francannet,Laëtitia Lambert,Aline Saunier,F. Verneau,Philippe Jonveaux
标识
DOI:10.1136/jmg.2009.067355
摘要
Background The FOXG1 gene has been recently implicated in the congenital form of Rett syndrome (RTT). It encodes the fork-head box protein G1, a winged-helix transcriptional repressor with expression restricted to testis and brain, where it is critical for forebrain development. So far, only two point mutations in FOXG1 have been reported in females affected by the congenital form of RTT. Aim To assess the involvement of FOXG1 in the molecular aetiology of classical RTT and related disorders. Methods The entire multi-exon coding sequence of FOXG1 was screened for point mutations and large rearrangements in a cohort of 35 MECP2/CDKL5 mutation-negative female patients including 31 classical and four congenital forms of RTT. Results Two different de novo heterozygous FOXG1 -truncating mutations were identified. The subject with the p.Trp308X mutation presented with a severe RTT-like neurodevelopmental disorder, whereas the p.Tyr400X allele was associated with a classical clinical RTT presentation. Conclusions These new cases give additional support to the genetic heterogeneity in RTT and help to delineate the clinical spectrum of the FOXG1 -related phenotypes. FOXG1 screening should be considered in the molecular diagnosis of RTT.
科研通智能强力驱动
Strongly Powered by AbleSci AI