对 7,000 名新生儿进行基于 WES 的筛查:在俄罗斯进行的试点研究。

IF 3.3 Q2 GENETICS & HEREDITY
HGG Advances Pub Date : 2024-10-10 Epub Date: 2024-07-19 DOI:10.1016/j.xhgg.2024.100334
Jekaterina Shubina, Ekaterina Tolmacheva, Dmitry Maslennikov, Taisiya Kochetkova, Irina Mukosey, Igor Sadelov, Andrey Goltsov, Ilya Barkov, Aleksey Ekimov, Margarita Rogacheva, Olga Stupko, Nadezhda Pavlova, Maria Kuznetsova, Alina Dokshukina, Grigory Vasiliev, Anna Bolshakova, Valeriia Kovalskaia, Anastasia Korovko, Ekaterina Pomerantseva, Polina Tsabai, Olga Buyanovskaya, Nadezhda Zaretskaya, Natalia Karetnikova, Elena Grebenshchikova, Anna Degtyareva, Ekaterina Bokerija, Alexey Kholin, Denis Rebrikov, Dmitry Degtyarev, Dmitriy Trofimov, Gennady Sukhih
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引用次数: 0

摘要

基于 WES 和 WGS 的诊断方法在遗传病患儿管理中的有效应用,以及 NGS 成本的迅速降低,使这种方法得以推广到新生儿基因筛查项目中。与传统的新生儿筛查相比,这种基于 NGS 的筛查大大增加了可检测疾病的数量,因为后者的目的是早期检测数量有限的先天性疾病。此外,基因检测还为疑似患者的家庭成员提供了新的可能性,因为许多导致成人发病的变异体都是由父母遗传的。然而,在健康儿童中进行基于 NGS 的筛查的想法引发了医疗和伦理诚信问题以及技术问题,包括对观察到的变异的解释。试点研究表明,家长和医疗专业人员都在向前迈进,并对这些新的可能性充满热情。然而,迄今为止,无论是参与人数还是所研究基因的数量都仅限于几百个,限制了潜在发现的范围。我们目前的研究(NCT05325749)包括 2021 年 2 月至 2023 年 5 月期间在我们中心出生的 7000 名表面健康的婴儿,这些婴儿接受了 2350 个基因致病变异的筛查。在 0.9% 表型正常的婴儿中观察到了与早发性疾病相关的具有临床意义的变异,这些疾病可以治疗、预防或通过及时的对症治疗缓解症状;2.1% 的受筛查新生儿被发现携带与渗透性降低或成人发病的单基因疾病和/或可变表达性相关的变异;0.3% 的新生儿存在染色体异常。在此,我们报告了我们的研究结果,并回答了有关假定健康新生儿变异的解释问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
WES-based screening of 7,000 newborns: A pilot study in Russia.

The effective implementation of whole-exome sequencing- and whole-genome sequencing-based diagnostics in the management of children affected with genetic diseases and the rapid decrease in the cost of next-generation sequencing (NGS) enables the expansion of this method to newborn genetic screening programs. Such NGS-based screening greatly increases the number of diseases that can be detected compared to conventional newborn screening, as the latter is aimed at early detection of a limited number of inborn diseases. Moreover, genetic testing provides new possibilities for family members of the proband, as many variants responsible for adult-onset conditions are inherited from the parents. However, the idea of NGS-based screening in healthy children raises issues of medical and ethical integrity as well as technical questions, including interpretation of the observed variants. Pilot studies have shown that both parents and medical professionals have moved forward and are enthused about these new possibilities. However, either the number of participants or the number of genes studied in previous investigations thus far has been limited to a few hundred, restricting the scope of potential findings. Our current study (NCT05325749) includes 7,000 apparently healthy infants born at our center between February 2021 and May 2023, who were screened for pathogenic variants in 2,350 genes. Clinically significant variants associated with early-onset diseases that can be treated, prevented, or where symptoms can be alleviated with timely introduced symptomatic therapy, were observed in 0.9% of phenotypically normal infants, 2.1% of the screened newborns were found to carry variants associated with reduced penetrance or monogenic diseases of adult-onset and/or variable expressivity, and 0.3% had chromosomal abnormalities. Here, we report our results and address questions regarding the interpretation of variants in newborns who were presumed to be healthy.

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来源期刊
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
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