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外显子组测序分析强调了未掩盖的隐性突变在部分外显率的拷贝数变异中的作用。

Whole-exome sequence analysis highlights the role of unmasked recessive mutations in copy number variants with incomplete penetrance.

机构信息

Service d'Histologie-Embryologie-Cytogénétique, Hôpital Necker-Enfants-Malades, Université Paris Descartes, 149, rue de Sèvres, 75015, Paris, France.

Institut IMAGINE, INSERM UMR S1163, Hôpital Necker-Enfants Malades, Paris, France.

出版信息

Eur J Hum Genet. 2018 Jun;26(6):912-918. doi: 10.1038/s41431-018-0124-4. Epub 2018 Feb 26.

DOI:10.1038/s41431-018-0124-4
PMID:29483668
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5974246/
Abstract

Several hypotheses have been proposed to explain the phenotypic variability between parent and offspring carrying the same genomic imbalance, including unmasking of a recessive variant by a chromosomal deletion. Here, 19 patients with neurodevelopmental disorders harboring a rare deletion inherited from a healthy parent were investigated by whole-exome sequencing to search for SNV on the contralateral segment. This strategy allowed us to identify a candidate variant in two patients in the NUP214 and NCOR1 genes. This result demonstrates that the analysis of the genes included in non-deleted contralateral allele is a key point in the etiological investigation of patients harboring a deletion inherited from a parent. Finally, this strategy is also an interesting approach to identify new recessive intellectual disability genes.

摘要

已经提出了几种假说来解释携带相同基因组不平衡的父母和子女之间的表型变异性,包括由染色体缺失掩盖隐性变异。在这里,通过全外显子组测序研究了 19 名携带由健康父母遗传的罕见缺失的神经发育障碍患者,以寻找对侧片段上的 SNV。这种策略使我们能够在 NUP214 和 NCOR1 基因的两名患者中鉴定出候选变异。这一结果表明,对包含在未缺失的对侧等位基因中的基因进行分析是对从父母遗传缺失的患者进行病因学研究的关键点。最后,这种策略也是识别新的隐性智力残疾基因的一种有趣方法。

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