基于捕获的产前无细胞 DNA 筛查常染色体隐性非综合征听力损失的方法。

IF 2.7 2区医学 Q2 GENETICS & HEREDITY

Prenatal Diagnosis Pub Date : 2024-08-01 Epub Date: 2024-03-15 DOI:10.1002/pd.6550

Qian Mu, Ling Bai, Bing Xu, Huawen Du, Zhaoyun Jiang, Shasha Huang, Bo Gao, Qixi Wu, Hanqing Zhao, Pu Dai, Yi Jiang

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引用次数: 0

摘要

研究目的本研究旨在开发并验证一种产前无细胞DNA（cfDNA）筛查方法，该方法利用基于捕获的富集技术对胎儿常染色体隐性遗传疾病进行基因分型。该方法适用于常染色体隐性非综合征听力损失（ARNSHL）高风险孕妇，以评估其准确性和有效性：方法：该检测方法采用基于捕获的下一代测序方法测量孕妇血样中白细胞 DNA 和 cfDNA 的等位基因数。然后应用二项式模型以最大似然法推断胎儿的基因型。研究共纳入了 94 对 GJB2 或 SLC26A4 中 ARNSHL 变体携带者的怀孕夫妇。将使用这种筛查方法推断出的胎儿基因型与使用羊膜腔穿刺术进行基因诊断的结果进行了比较：结果：在94对夫妇中，有65对携带一个以上的变异体，从而推断出胎儿的170个单核苷酸多态性（SNP）位点。在170个胎儿SNP基因型中，150个（88.2%）具有高置信度调用，其中139个（92.7%）与羊膜腔穿刺结果所获得的基因型相匹配。在其余 20 个（11.8%）低置信度调用的病例中，只有 14 个（70.0%）与羊膜腔穿刺的基因诊断结果一致。母体基因型为野生型同卵双生的位点的吻合率为 100%。不一致是有位点偏倚的，每个位点都显示出一致的不一致方向。基因诊断共鉴定出 19 个野生型同源基因、46 个杂合基因、19 个复合杂合基因和 10 个致病性同源基因。这种筛查方法对 81.9%（77/94）的胎儿进行了正确的基因分型，对正确识别 ARNSHL 的灵敏度为 89.7%，特异度为 89.2%：结论：这种基于捕获的 cfDNA 产前筛查方法在常染色体隐性遗传病的胎儿基因分型中显示出强大的潜力。

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A capture-based method of prenatal cell-free DNA screening for autosomal recessive non-syndromic hearing loss.

Objective: This study aimed to develop and validate a prenatal cell-free DNA (cfDNA) screening method that uses capture-based enrichment to genotype fetal autosomal recessive disorders. This method was applied in pregnancies at high risk of autosomal recessive non-syndromic hearing loss (ARNSHL) to assess its accuracy and effectiveness.

Methods: This assay measured the allele counts in both white blood cell DNA and cfDNA from the blood samples of pregnant women using a capture-based next-generation sequencing method. It then applied a binomial model to infer the fetal genotypes with the maximum likelihood. Ninety-four pregnant couples that were carriers of variants of ARNSHL in GJB2 or SLC26A4 were enrolled. The fetal genotypes deduced using this screening method were compared with the results of genetic diagnosis using amniocentesis.

Results: Of the 94 couples, 65 carried more than one variant, resulting in 170 single-nucleotide polymorphism (SNP) loci to be inferred in the fetuses. Of the 170 fetal SNP genotypes, 150 (88.2%) had high confidence calls and 139 (92.7%) of these matched the genotypes obtained by amniocentesis result. Out of the remaining 20 (11.8%) cases with low-confidence calls, only 14 (70.0%) were concordant with genetic diagnosis using amniocentesis. The concordance rate was 100% for sites where the maternal genotype was wild-type homozygous. The discordance was site-biased, with each locus showing a consistent direction of discordance. Genetic diagnosis identified a total of 19 wild-type homozygotes, 46 heterozygotes, 19 compound heterozygotes, and 10 pathogenic homozygotes. This screening method correctly genotyped 81.9% (77/94) of fetuses and demonstrated a sensitivity of 89.7% and a specificity of 89.2% for correctly identifying ARNSHL.

Conclusion: This capture-based method of prenatal screening by cfDNA demonstrated strong potential for fetal genotyping of autosomal recessive disorders.

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来源期刊

Prenatal Diagnosis 医学-妇产科学

CiteScore

5.80

自引率

13.30%

发文量

204

审稿时长

2 months

期刊介绍： Prenatal Diagnosis welcomes submissions in all aspects of prenatal diagnosis with a particular focus on areas in which molecular biology and genetics interface with prenatal care and therapy, encompassing: all aspects of fetal imaging, including sonography and magnetic resonance imaging; prenatal cytogenetics, including molecular studies and array CGH; prenatal screening studies; fetal cells and cell-free nucleic acids in maternal blood and other fluids; preimplantation genetic diagnosis (PGD); prenatal diagnosis of single gene disorders, including metabolic disorders; fetal therapy; fetal and placental development and pathology; development and evaluation of laboratory services for prenatal diagnosis; psychosocial, legal, ethical and economic aspects of prenatal diagnosis; prenatal genetic counseling