Objective: To study the association between clinical phenotypes and genotypes in children with Becker muscular dystrophy (BMD)/Duchenne muscular dystrophy (DMD) so as to provide a theoretical basis for disease management, gene therapy, and prenatal diagnosis.
Methods: A retrospective analysis was performed for the clinical data and gene detection results of 52 children with BMD/DMD. Multiplex ligation-dependent probe amplification (MLPA) was used to detect the DMD gene. The children with negative results of MLPA were further screened by exon chip capture combined with next-generation sequencing (NGS). The mothers of 20 probands were validated by sequencing.
Results: The pathogenic genes for BMD/DMD were detected in 50 children by MLPA and NGS, with a detection rate of 96%. Among the 52 children, 36 (69%) had gene deletion, 7 (13%) had duplication, and 7 (13%) had micromutation. Among the 43 children with deletion/duplication, 32 had DMD and 11 had BMD; 37 children (86%) met the reading frame rule, among whom 27 (96%) had DMD and 10 (67%) had BMD. All 7 children with micromutation had DMD.
Conclusions: The reading frame rule has an extremely high predictive value for DMD but a limited predictive value for BMD.
目的: 探讨Becker/Duchenne肌营养不良(BMD/DMD)患儿的临床表型与基因型的关联性,为疾病的管理、基因治疗及产前诊断提供理论依据。
方法: 回顾性分析52例患儿的临床资料及基因检测结果,对52例患儿均采用多重连接探针扩增(MLPA)的方法检测DMD基因,对MLPA检测未发现基因异常的患儿采用外显子芯片捕获结合高通量测序技术(NGS)进行筛查;并对20例先证者的母亲进行了测序验证。
结果: 结合MLPA和NGS测序技术检测到50例患儿携带BMD/DMD致病基因,检出率为96%。其中,基因缺失36例(69%)、重复7例(13%)、微小突变7例(13%)。在43例存在基因缺失/重复的患儿中,DMD 32例,BMD 11例;37例(86%)符合阅读框架原则,其中DMD 27例(96%),BMD 10例(67%)。7例微小突变均为DMD。
结论: 阅读框架原则对DMD有极高预测价值,对BMD预测有限。