Characteristic genetic spectrum of primary ciliary dyskinesia in Japanese patients and global ethnic heterogeneity: population-based genomic variation database analysis

原发性睫状体运动障碍 遗传学 生物 错义突变 等位基因 遗传变异 拷贝数变化 外显子组测序 遗传异质性 基因 人口 1000基因组计划 外显子组 等位基因频率 基因组 基因型 单核苷酸多态性 突变 表型 医学 环境卫生 内科学 支气管扩张
作者
Yifei Xu,Guofei Feng,Taichi Yano,Sawako Masuda,Mizuho Nagao,Shimpei Gotoh,Makoto Ikejiri,Masaki Tanabe,Kazuhiko Takeuchi
出处
期刊:Journal of Human Genetics [Springer Nature]
卷期号:68 (7): 455-461 被引量:14
标识
DOI:10.1038/s10038-023-01142-4
摘要

Primary ciliary dyskinesia (PCD) is a hereditary disease caused by pathogenic variants in genes associated with motile cilia. Some variants responsible for PCD are reported to be ethnic-specific or geographical-specific. To identify the responsible PCD variants of Japanese PCD patients, we performed next-generation sequencing of a panel of 32 PCD genes or whole-exome sequencing in 26 newly identified Japanese PCD families. We then combined their genetic data with those from 40 Japanese PCD families reported previously, for an overall analysis of 66 unrelated Japanese PCD families. We conducted Genome Aggregation Database and TogoVar database analyses to reveal the PCD genetic spectrum of the Japanese population and compare with other ethnic groups worldwide. We identified 22 unreported variants among the 31 patients in the 26 newly identified PCD families, including 17 deleterious variants estimated to cause lack of transcription or nonsense-mediated mRNA decay and 5 missense mutations. In all 76 PCD patients from the 66 Japanese families, we identified 53 variants on 141 alleles in total. Copy number variation in DRC1 is the most frequent variant in Japanese PCD patients, followed by DNAH5 c.9018C>T. We found 30 variants specific to the Japanese population, of which 22 are novel. Furthermore, 11 responsible variants in the Japanese PCD patients are common in East Asian populations, while some variants are more frequent in other ethnic groups. In conclusion, PCD is genetically heterogeneous between different ethnicities, and Japanese PCD patients have a characteristic genetic spectrum.
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