Penetrance, variable expressivity and monogenic neurodevelopmental disorders

IF 1.6 4区医学 Q3 GENETICS & HEREDITY

European journal of medical genetics Pub Date : 2024-03-05 DOI:10.1016/j.ejmg.2024.104932

Servane de Masfrand , Benjamin Cogné , Mathilde Nizon , Wallid Deb , Alice Goldenberg , François Lecoquierre , Gaël Nicolas , Marie Bournez , Antonio Vitobello , Frédéric Tran Mau-Them , Gwenaël le Guyader , Frédéric Bilan , Peter Bauer , Christiane Zweier , Juliette Piard , Laurent Pasquier , Stéphane Bézieau , Bénédicte Gerard , Laurence Faivre , Pascale Saugier-Veber , Bertrand Isidor

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引用次数: 0

Abstract

Purpose

Incomplete penetrance is observed for most monogenic diseases. However, for neurodevelopmental disorders, the interpretation of single and multi-nucleotide variants (SNV/MNVs) is usually based on the paradigm of complete penetrance.

Method

From 2020 to 2022, we proposed a collaboration study with the French molecular diagnosis for intellectual disability network. The aim was to recruit families for whom the index case, diagnosed with a neurodevelopmental disorder, was carrying a pathogenic or likely pathogenic variant for an OMIM morbid gene and inherited from an asymptomatic parent. Grandparents were analyzed when available for segregation study.

Results

We identified 12 patients affected by a monogenic neurodevelopmental disorder caused by likely pathogenic or pathogenic variant (SNV/MNV) inherited from an asymptomatic parent. These genes were usually associated with de novo variants. The patients carried different variants (1 splice-site variant, 4 nonsense and 7 frameshift) in 11 genes: CAMTA1, MBD5, KMT2C, KMT2E, ZMIZ1, MN1, NDUFB11, CUL3, MED13, ARID2 and RERE. Grandparents have been tested in 6 families, and each time the variant was confirmed de novo in the healthy carrier parent.

Conclusion

Incomplete penetrance for SNV and MNV in neurodevelopmental disorders might be more frequent than previously thought. This point is crucial to consider for interpretation of variants, family investigation, genetic counseling, and prenatal diagnosis. Molecular mechanisms underlying this incomplete penetrance still need to be identified.

查看原文本刊更多论文

渗透性、可变表现性和单基因神经发育障碍。

目的：大多数单基因疾病都存在不完全渗透性。然而，对于神经发育性疾病，单核苷酸和多核苷酸变异（SNV/MNVs）的解释通常基于完全渗透性范式：从 2020 年到 2022 年，我们提议与法国智障分子诊断网络合作开展一项研究。研究的目的是招募那些被诊断出患有神经发育障碍的病例携带有致病或可能致病的OMIM病态基因变异，并由无症状的父母遗传的家庭。如果可以进行分离研究，则对祖父母进行分析：结果：我们发现了 12 例由无症状父母遗传的可能致病或致病变异（SNV/MNV）引起的单基因神经发育障碍患者。这些基因通常与从头变异有关。患者的 11 个基因携带不同的变异（1 个剪接位点变异、4 个无义变异和 7 个帧移位变异）：CAMTA1、MBD5、KMT2C、KMT2E、ZMIZ1、MN1、NDUFB11、CUL3、MED13、ARID2 和 RERE。对 6 个家庭的祖父母进行了检测，每次都在健康的携带者父母中从头确认了该变异：结论：神经发育性疾病中 SNV 和 MNV 的不完全渗透性可能比以前认为的更为常见。这一点对于解释变异、家庭调查、遗传咨询和产前诊断至关重要。这种不完全渗透性的分子机制仍有待确定。

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

European journal of medical genetics 医学-遗传学

CiteScore

4.10

自引率

0.00%

发文量

193

审稿时长

66 days

期刊介绍： The European Journal of Medical Genetics (EJMG) is a peer-reviewed journal that publishes articles in English on various aspects of human and medical genetics and of the genetics of experimental models. Original clinical and experimental research articles, short clinical reports, review articles and letters to the editor are welcome on topics such as : • Dysmorphology and syndrome delineation • Molecular genetics and molecular cytogenetics of inherited disorders • Clinical applications of genomics and nextgen sequencing technologies • Syndromal cancer genetics • Behavioral genetics • Community genetics • Fetal pathology and prenatal diagnosis • Genetic counseling.