摘要
目的:应用二核苷酸重复多态Duchenne型肌营养不良症(DMD)基因诊断,探讨DMD产前基因诊断方案及其可行性。方法:在应用聚合酶链反应(PCR)初步分析Dystrophin基因内含子49和45的(CA)n多态分布的基础上,以Dystrophin基因5′端(CA)n多态和内含子45,49,50以及3′端(CA)n多态为遗传标记,单体型连锁分析的同时直接检测缺失相结合的方法。结果:Dystrophin基因内含子49和45的(CA)n多态共检测到7个和6个等位片段,实际检出的杂合子率为86.6%和73%;在东北地区首次成功地完成了8个家系9例DMD产前基因诊断。结论:该方法不分缺失型和非缺失型一步完成诊断,是临床产前基因诊断较理想的方案。
Objective:WT5BZUsing dinucleotide repeat polymorphism in the dystrophin gene as
markers,we intended to improve prenatal diagnosis for Duchenne muscular dystroph (DMD)
families and to evaluate its feasibility. Methods: We took dinucleotide repeat polymorphism
located in 3 end and 5 end and introns 454950 of the dystrophin gene as markers, and
combined haplotype linkage analysis with direct deletional detection by PCR to diagnose the
Duchenne muscular dystrophy.Results: Seven and six allelic fragments were found out in
introns 49 and 45, respectively. The actually detected rate of heterozygosities was 86.6% and
73%,respectively.We first successfully finished prenatal gene diagnosis of nine cases in eight
DMD families. Conclusion: We efficiently finished prenatal gene diagnosis in DMD just by one
step,no matter the gene is deletion or not. This strategy would be a valuable method for the
clinical prenatal diagnosis.
出处
《中国医科大学学报》
CAS
CSCD
北大核心
1999年第3期186-188,共3页
Journal of China Medical University
基金
卫生部科研基金
关键词
DUCHENNE型
肌营养不良症
二核苷酸
产前诊断
Duchenne muscular dystrophy
dinucleotide repeat
polymorphism
prenatal diagnosis
dystrophin gene
