Nanopore Third-Generation Sequencing for Comprehensive Analysis of Hemoglobinopathy Variants

纳米孔测序 血红蛋白病 遗传学 生物 计算生物学 DNA测序 医学 DNA 溶血性贫血 内科学
作者
Weilun Huang,Shoufang Qu,Qiongzhen Qin,Yang Xu,Wenbo Han,Yun‐Wen Lai,Jiaqi Chen,Shihao Zhou,Xuexi Yang,Wanjun Zhou
出处
期刊:Clinical Chemistry [Oxford University Press]
卷期号:69 (9): 1062-1071 被引量:3
标识
DOI:10.1093/clinchem/hvad073
摘要

Abstract Background Oxford Nanopore Technology (ONT) third-generation sequencing (TGS) is a versatile genetic diagnostic platform. However, it is nonetheless challenging to prepare long-template libraries for long-read TGS, particularly the ONT method for analysis of hemoglobinopathy variants involving complex structures and occurring in GC-rich and/or homologous regions. Methods A multiplex long PCR was designed to prepare library templates, including the whole-gene amplicons for HBA2/1, HBG2/1, HBD, and HBB, as well as the allelic amplicons for targeted deletions and special structural variations. Library construction was performed using long-PCR products, and sequencing was conducted on an Oxford Nanopore MinION instrument. Genotypes were identified based on integrative genomics viewer (IGV) plots. Results This novel long-read TGS method distinguished all single nucleotide variants and structural variants within HBA2/1, HBG2/1, HBD, and HBB based on the whole-gene sequence reads. Targeted deletions and special structural variations were also identified according to the specific allelic reads. The result of 158 α-/β-thalassemia samples showed 100% concordance with previously known genotypes. Conclusions This ONT TGS method is high-throughput, which can be used for molecular screening and genetic diagnosis of hemoglobinopathies. The strategy of multiplex long PCR is an efficient strategy for library preparation, providing a practical reference for TGS assay development.
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