303个中国家庭营养不良蛋白病的产前诊断及细胞遗传学分析

Mengmeng Li, N. Hao, F. Yao, Wei-min Zhang, Jing Zhou, Li Tan, Z. Qiu, Juntao Liu
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摘要

摘要目的:本研究旨在提供303个中国家庭的杜氏肌营养不良(DMD)突变谱信息,并为DMD/Becker肌营养不良的遗传咨询和产前诊断提供5年的临床经验。方法:在这项回顾性队列研究中,2014年1月至2018年12月,303名有DMD/Becker肌营养不良出生史的孕妇在北京协和医院接受了多重结扎依赖性探针扩增和Sanger测序的产前诊断。孕妇的平均年龄为(33.0 ± 4.1)岁。进行核型分析以排除胎儿异常核型。结果:303例先证者DMD基因突变检出率为(296/303)97.7%,其中7个家系遗传诊断为阴性。突变谱包括288/303(95.0%)的大突变和8/303(2.6%)的小突变。对204名孕妇进行了携带者检测,其中108名母亲与家族先证者具有相同的突变。在305例接受产前诊断的妊娠中,173例男性胎儿中有55例受到影响。我们还进行了核型分析,发现了三种21三体的异常核型。通过进一步分析,我们甚至在同一胎儿中发现了一个DMD基因突变和21三体的胎儿。我们还发现了两次种系嵌合体。结论:本研究揭示了303例先证者和305例胎儿的分布和突变特征。此外,考虑到母系-生殖系嵌合体的可能性,无论先证者的血液中是否携带致病突变,都应建议对其进行产前诊断。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prenatal Diagnosis of Dystrophinopathy and Cytogenetic Analysis in 303 Chinese Families
Abstract Objective: This study was to supply information of the Duchenne muscular dystrophy (DMD) mutational spectrum in 303 Chinese families and further offer 5-year clinical experience of DMD/Becker muscular dystrophy genetic counseling and prenatal diagnosis. Methods: In this retrospective cohort study, three hundred and five pregnancies in 303 pregnant women who has a birth history of DMD/Becker muscular dystrophy patients underwent prenatal diagnosis using multiplex ligation-dependent probe amplification followed by Sanger sequencing between January 2014 and December 2018 at Peking Union Medical College Hospital. The mean age of pregnant women was (33.0 ± 4.1) years old. Karyotype analysis was performed to exclude fetal abnormal karyotype. Results: The detection rate of DMD gene mutation in 303 probands was (296/303) 97.7% with seven families having a negative genetic diagnosis. The mutational spectrum comprised of large arrangements in 288/303 (95.0%) and small mutations in 8/303 (2.6%). Carrier testing was performed among 204 pregnant women among whom, 108 mothers had the same mutation as family proband. Of the 305 pregnancies underwent prenatal diagnosis, 55 of 173 male fetuses were affected. We also performed karyotype analysis and found three abnormal karyotypes of trisomy 21. We even found a fetus with DMD gene mutation and trisomy 21 in a same fetus by further analysis. We also identified two times of germline mosaicism. Conclusion: This study demonstrated the distribution and mutation profile of 303 probands and 305 fetuses. Furthermore, considering the possbility of maternl germilne mosaicism, prenatal diagnosis should be suggested to mothers with a proband whether they carry the causative mutation in their blood or not.
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