Clinical use of whole exome sequencing in children with developmental delay/intellectual disability

IF 2.3 4区 医学 Q2 PEDIATRICS Pediatrics and Neonatology Pub Date : 2024-09-01 DOI:10.1016/j.pedneo.2023.05.015
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Abstract

Background

Identifying the underlying etiology of developmental delay/intellectual disability (DD/ID) is challenging but important. The genetic diagnosis of unexplained DD/ID helps in the treatment and prognosis of the disability in patients. In this study, we reported our experience of using whole exome sequencing (WES) of children with unexplained DD/ID.

Methods

We conducted a retrospective analysis of WES results of children under 19 years of age with unexplained DD/ID between January 2020 and December 2021. The demographic data of all patients and variants identified through WES were evaluated. Furthermore, we evaluated the clinical characteristics that influenced the identification of genetic causes.

Results

Forty-one patients with DD/ID were included, of whom 21 (51.2 %) were male. The average age at symptom onset was 1.6 ± 1.3 years, and the duration from symptom onset to diagnosis was 3.1 ± 3.7 years. Hypotonia was the most common symptom (17 patients, 41.5 %), and epilepsy was confirmed in 10 patients (24.4 %). Twenty-two pathogenic/likely pathogenic variants were identified in 20 patients, and three variants of uncertain significance were identified in three patients. Family-based trio Sanger sequencing for candidate variants of 12 families was conducted; 10 variants were de novo, one variant paternally inherited, and two variants compound heterozygous. The diagnostic yield of WES for DD/ID was 48.8 % and was significantly high in patients with an early onset of DD/ID and facial dysmorphism. In contrast, patients with autism spectrum disorder (ASD) were more likely to have negative WES results compared with others without ASD.

Conclusion

The diagnostic yield of WES was 48.8 %. We conclude that patients’ characteristics, such as dysmorphic features and the age of symptom onset, can predict the likelihood that WES will identify a causal variant of a phenotype.

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全外显子组测序在发育迟缓/智力障碍儿童中的临床应用
背景确定发育迟缓/智力障碍(DD/ID)的潜在病因具有挑战性,但却非常重要。不明原因发育迟缓/智力障碍的基因诊断有助于患者的治疗和预后。我们对 2020 年 1 月至 2021 年 12 月期间 19 岁以下不明原因 DD/ID 儿童的全外显子组测序(WES)结果进行了回顾性分析。我们评估了所有患者的人口统计学数据以及通过 WES 鉴定出的变异体。此外,我们还评估了影响遗传原因鉴定的临床特征。结果共纳入 41 名 DD/ID 患者,其中 21 名(51.2%)为男性。患者发病时的平均年龄为(1.6 ± 1.3)岁,从发病到确诊的持续时间为(3.1 ± 3.7)年。肌张力低下是最常见的症状(17 名患者,41.5%),10 名患者(24.4%)被确诊为癫痫。在20名患者中发现了22个致病/可能致病变异,在3名患者中发现了3个意义不明的变异。对 12 个家庭的候选变异体进行了基于家庭的三组 Sanger 测序;其中 10 个变异体为新发变异体,1 个变异体为父系遗传变异体,2 个变异体为复合杂合变异体。WES对DD/ID的诊断率为48.8%,在早发性DD/ID和面部畸形患者中诊断率明显较高。相比之下,自闭症谱系障碍(ASD)患者的 WES 结果为阴性的几率要高于其他无自闭症谱系障碍的患者。我们得出的结论是,患者的特征(如畸形特征和发病年龄)可以预测 WES 发现表型因果变异的可能性。
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来源期刊
CiteScore
3.10
自引率
0.00%
发文量
170
审稿时长
48 days
期刊介绍: Pediatrics and Neonatology is the official peer-reviewed publication of the Taiwan Pediatric Association and The Society of Neonatology ROC, and is indexed in EMBASE and SCOPUS. Articles on clinical and laboratory research in pediatrics and related fields are eligible for consideration.
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