Potentially Missed Diagnoses in Prenatal Versus Postnatal Exome Sequencing in the Lack of Informative Phenotype: Lessons Learned From a Postnatal Cohort.

IF 2.7 2区医学 Q2 GENETICS & HEREDITY

Prenatal Diagnosis Pub Date : 2024-09-05 DOI:10.1002/pd.6659

Dana Brabbing-Goldstein, Lily Bazak, Noa Ruhrman-Shahar, Gabriel Arie Lidzbarsky, Naama Orenstein, Marina Lifshiz-Kalis, Nurit Asia-Batzir, Yael Goldberg, Lina Basel-Salmon

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引用次数: 0

Abstract

Objective: To investigate how many novel pathogenic (P) and likely pathogenic (LP) nonprotein-truncating or noncanonical splicing variants would be classified as variants of unknown significance (VUS) if they were detected in fetuses without abnormalities.

Methods: The study included 156 patients with neurodevelopmental disorders diagnosed through postnatal exome sequencing. Causative P/LP nonprotein-truncating and noncanonical splicing variants were retrospectively reclassified in cases without specific prenatal manifestations, disregarding postnatal symptoms.

Results: Of the 156 patients, 72 had a nontruncating or noncanonical splicing variant. Six patients were excluded for having more than one possible causative variant. Twelve patients had prenatal malformations known to be associated with the diagnosed disorder; therefore, variant interpretation remained unchanged. In 33 of the 54 remaining cases, the variant had been previously reported as P/LP. Reclassification of the other 21 LP/P variants revealed that 16 would have been classified as VUS if detected prenatally.

Conclusion: In our cohort, ∼24% (16/66) of causative nonprotein-truncating/noncanonical splicing variants would have been classified as VUS if sequencing had been conducted during pregnancy. The potential for false-negative results, stemming from limitations in the phenotypic information available prenatally, should be discussed with prospective parents. The criteria for classifying and reporting variants in the prenatal setting may require adjustment.

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在缺乏信息表型的情况下，产前与产后外显子组测序的潜在漏诊：从产后队列中汲取的教训》。

目的调查如果在无异常的胎儿中检测到新的致病性（P）和可能致病性（LP）非蛋白截断或非典型剪接变异，有多少变异会被归类为意义不明的变异（VUS）：研究纳入了156名通过产后外显子组测序确诊的神经发育障碍患者。在没有特定产前表现的病例中，不考虑产后症状，对致病的P/LP非蛋白截断变异和非典型剪接变异进行了回顾性重新分类：结果：在 156 例患者中，72 例有非截断或非典型剪接变异。6名患者因有一个以上可能的致病变体而被排除在外。12名患者的产前畸形已知与所诊断的疾病有关；因此，对变异的解释保持不变。在剩余的 54 个病例中，有 33 个病例的变异先前被报告为 P/LP。对其他21个LP/P变异体进行重新分类后发现，如果在产前发现，其中16个变异体会被归类为VUS：结论：在我们的队列中，如果在孕期进行测序，24%（16/66）的致病性非蛋白截断/非调和剪接变异会被归类为 VUS。由于产前可获得的表型信息有限，可能会出现假阴性结果，因此应与准父母进行讨论。产前变异的分类和报告标准可能需要调整。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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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