Clinical diagnosis of genetic disorders at both single-nucleotide and chromosomal levels based on BGISEQ-500 platform.
Yanqiu LiuLiangwei MaoHui HuangWei LiJianfen ManWenqian ZhangLina WangLong LiYan SunTeng ZhaiXueqin GuoLique DuJin HuangHao LiYang WanXiaoming WeiPublished in: Human genome variation (2023)
Most variations in the human genome refer to single-nucleotide variation (SNV), small fragment insertions and deletions, and genomic copy number variation (CNV). Many human diseases including genetic disorders are associated with variations in the genome. These disorders are often difficult to be diagnosed because of their complex clinical conditions, therefore, an effective detection method is needed to facilitate clinical diagnosis and prevent birth defects. With the development of high-throughput sequencing technology, the method of targeted sequence capture chip has been extensively used owing to its high throughput, high accuracy, fast speed, and low cost. In this study, we designed a chip that potentially captured the coding region of 3043 genes associated with 4013 monogenic diseases, with an addition of 148 chromosomal abnormalities that can be identified by targeting specific regions. To assess the efficiency, a strategy of combining the BGISEQ500 sequencing platform with the designed chip was utilized to screen variants in 63 patients. Eventually, 67 disease-associated variants were found, 31 of which were novel. The results of the evaluation test also show that this combined strategy complies with the requirements of clinical testing and has proper clinical application value.
Keyphrases
- copy number
- high throughput
- mitochondrial dna
- genome wide
- endothelial cells
- single cell
- low cost
- dna methylation
- end stage renal disease
- gene expression
- peritoneal dialysis
- multidrug resistant
- circulating tumor cells
- ejection fraction
- pregnant women
- induced pluripotent stem cells
- amino acid
- drug delivery
- pregnancy outcomes