176 名西班牙神经发育障碍儿童的全外显子组测序和基于面板的分析:重点是自闭症谱系障碍和/或智力残疾/全面发育迟缓。
Whole Exome Sequencing and Panel-Based Analysis in 176 Spanish Children with Neurodevelopmental Disorders: Focus on Autism Spectrum Disorder and/or Intellectual Disability/Global Developmental Delay.
机构信息
Escuela Internacional de Doctorado, Rey Juan Carlos University, Alcorcón Campus, 28922 Madrid, Spain.
Faculty of Biomedical and Health Sciences, Universidad Europea de Madrid, Villaviciosa de Odón, 28670 Madrid, Spain.
出版信息
Genes (Basel). 2024 Oct 11;15(10):1310. doi: 10.3390/genes15101310.
BACKGROUND
Neurodevelopmental disorders (NDDs) represent a significant challenge in pediatric genetics, often requiring advanced diagnostic tools for the accurate identification of genetic variants.
OBJECTIVES
To determine the diagnostic yield of whole exome sequencing (WES) with targeted gene panels in children with neurodevelopmental disorders (NDDs).
METHODS
This observational, prospective study included a total of 176 Spanish-speaking pediatric patients with neurodevelopmental disorders (NDDs), encompassing intellectual disability (ID), global developmental delay (GDD), and/or autism spectrum disorder (ASD). Participants were recruited from January 2019 to January 2023 at a University Hospital in Madrid, Spain. Clinical and sociodemographic variables were recorded, along with genetic study results. The age range of the subjects was 9 months to 16 years, and the percentage of males was 72.1%. The diagnostic yield of whole exome sequencing (WES) was calculated both before and after parental testing via Sanger DNA sequencing.
RESULTS
The study included 176 children: 67 (38.1%) with ID, 62 (35.2%) with ASD, and 47 (26.7%) with ASD + ID. The diagnostic yield of proband-only exome sequencing was 12.5% (22/176). By group, the diagnostic yield of proband-only exome sequencing was 3.2% in the ASD, 12.7% in the ASD + ID, and 20.8% in the ID group. Variants of uncertain significance (VUS) were found in 39.8% (70/176). After parental testing, some variants were reclassified as "likely pathogenic", increasing the diagnostic yield by 4.6%, with an overall diagnostic yield of 17.1%. Diagnostic yield was higher in patients with syndromic ID (70.6%% vs. 29.4%; 0.036).
CONCLUSIONS
A sequential approach utilizing WES followed by panel-based analysis, starting with the index case and, when appropriate, including the parents, proves to be a cost-effective strategy. WES is particularly suitable for complex conditions, as it allows for the identification of potentially causative genes beyond those covered by targeted panels, providing a more comprehensive analysis. Including parental testing enhances the diagnostic yield and improves accuracy, especially in cases with variants of uncertain significance (VUS), thereby advancing our understanding of NDDs.
背景
神经发育障碍(NDD)是儿科遗传学的一个重大挑战,通常需要先进的诊断工具来准确识别遗传变异。
目的
确定全外显子组测序(WES)与靶向基因panel 在神经发育障碍(NDD)儿童中的诊断效果。
方法
这是一项观察性、前瞻性研究,共纳入 176 名患有神经发育障碍(NDD)的西班牙语儿童,包括智力障碍(ID)、全面发育迟缓(GDD)和/或自闭症谱系障碍(ASD)。参与者于 2019 年 1 月至 2023 年 1 月在西班牙马德里的一家大学医院招募。记录了临床和社会人口学变量以及遗传研究结果。研究对象的年龄范围为 9 个月至 16 岁,男性占 72.1%。分别计算了在进行父母 Sanger DNA 测序之前和之后,全外显子组测序(WES)的诊断效果。
结果
该研究共纳入 176 名儿童:67 名(38.1%)有 ID,62 名(35.2%)有 ASD,47 名(26.7%)有 ASD+ID。仅对先证者进行外显子组测序的诊断效果为 12.5%(22/176)。按组计算,仅对先证者进行外显子组测序的诊断效果在 ASD 组为 3.2%,在 ASD+ID 组为 12.7%,在 ID 组为 20.8%。不确定意义的变异(VUS)占 39.8%(70/176)。在进行父母测试后,一些变异被重新归类为“可能致病性”,将诊断效果提高了 4.6%,总诊断效果为 17.1%。在有综合征性 ID 的患者中,诊断效果更高(70.6% vs. 29.4%;0.036)。
结论
采用 WES 结合基于panel 的分析的序贯方法,先对先证者进行检测,必要时对父母进行检测,是一种具有成本效益的策略。WES 特别适用于复杂疾病,因为它可以识别靶向panel 之外的潜在致病基因,提供更全面的分析。纳入父母测试可以提高诊断效果和准确性,尤其是在有不确定意义的变异(VUS)的情况下,从而加深我们对 NDD 的认识。
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