Genetic characterization and screening of congenital adrenal hyperplasia by long-read sequencing in a cohort of 21,239 newborns

先天性肾上腺增生 等位基因频率 医学 遗传学 人口 基因座(遗传学) 等位基因 载波测试 基因检测 队列 生物 人类遗传学 置信区间 入射(几何) 医学遗传学 遗传咨询 遗传变异 生物信息学 肾上腺疾病 索引 嵌合体(遗传学) 外显子组测序 儿科 产前诊断 DNA测序 一致性 遗传诊断 单倍型 生殖技术 次等位基因频率 内科学
作者
Desheng Liang,Min Zhu,Qiaowei Liang,Rong Qiang,Lei Yu,Shiyi Xu,Mo Li,Jieping Song,Yulin Zhou,Xiaoyan He,Yonglan Huang,Hua Jin,Jianqiang Tan,Hui Liu,Aihua Xia,Yingdi Liu,Peisen Liu,Zhuo Li,Ruifang Wang,Dongjuan Wang
出处
期刊:Genome Medicine [BioMed Central]
卷期号:18 (1): 15-15 被引量:2
标识
DOI:10.1186/s13073-025-01594-7
摘要

Comprehensive genetic characterization and screening for congenital adrenal hyperplasia (CAH) have not yet been achieved at the population level because of the complexity of the CYP21A2 locus. This prospective study incorporated long-read sequencing (LRS) into the current first-tier biochemical newborn screening (NBS) to comprehensively characterize the variant spectrum of CYP21A2, fully investigate the carrier frequency and expected incidence of classic and non-classic CAH (NCCAH), and evaluate the clinical feasibility of genetic NBS for CAH. A total of 21,239 newborns were consecutively recruited from 11 centers across China between June 2023 and May 2024. All the participants underwent biochemical and genetic NBS. In vitro enzymatic activity and minigene assays were performed to determine the pathogenicity of novel variants. A 30.8-kb long amplicon, followed by LRS, was performed to determine the phasing of duplication chimera and single-nucleotide variations (SNVs) and indels in CYP21A2. Eligible genetic screening results were obtained for 21,234 (99.98%) newborns. The allele frequencies of duplications and deletions at the CYP21A2 locus were 4.51% and 0.15%, respectively. In vitro functional analysis and LRS-based phasing were performed to precisely determine carrier alleles, setting an overall frequency of 1.67% (711/42468, 95% confidence interval (CI): 1.55–1.80%), with 0.75% (320/424268, 95% CI: 0.67–0.84%) and 0.92% (391/42468, 95% CI: 0.83–1.01%) for classic and NC carriers, respectively. Notably, hotspot variants including SNVs/indels caused by microgene conversion and 30-kb deletions caused by unequal crossover accounted for 84.0% (597/711), whereas rare variants comprised as high as 16.0% (114/711) of all variants. The expected incidence of classic CAH according to allele frequency was 1/17613. The expected incidence of NCCAH in Chinese population (1/4474) was significantly lower than that in US Ashkenazi Jews (1/133) and Caucasians (1/337), mainly owing to the different allele frequencies of the NC variant CYP21A2:c.844G > T. Biochemical NBS identified 106 (0.50%) positive samples with a positive predictive value of 0.94% (1/106). LRS accurately identified the one case of classic CAH, with no false positives. Our findings provide a population-level carrier frequency and incidence estimates with a comprehensive landscape of the CYP21A2 locus, and demonstrate the effectiveness of first-tier LRS-based genetic NBS for CAH.
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