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NR4A2 的从头变异与神经发育障碍和癫痫有关。

De novo variants of NR4A2 are associated with neurodevelopmental disorder and epilepsy.

机构信息

Department of Genetics, University Medical Centre Utrecht, Utrecht, The Netherlands.

Center for Individualized Medicine, Mayo Clinic, Rochester, MN, USA.

出版信息

Genet Med. 2020 Aug;22(8):1413-1417. doi: 10.1038/s41436-020-0815-4. Epub 2020 May 5.

Abstract

PURPOSE

This study characterizes the clinical and genetic features of nine unrelated patients with de novo variants in the NR4A2 gene.

METHODS

Variants were identified and de novo origins were confirmed through trio exome sequencing in all but one patient. Targeted RNA sequencing was performed for one variant to confirm its splicing effect. Independent discoveries were shared through GeneMatcher.

RESULTS

Missense and loss-of-function variants in NR4A2 were identified in patients from eight unrelated families. One patient carried a larger deletion including adjacent genes. The cases presented with developmental delay, hypotonia (six cases), and epilepsy (six cases). De novo status was confirmed for eight patients. One variant was demonstrated to affect splicing and result in expression of abnormal transcripts likely subject to nonsense-mediated decay.

CONCLUSION

Our study underscores the importance of NR4A2 as a disease gene for neurodevelopmental disorders and epilepsy. The identified variants are likely causative of the seizures and additional developmental phenotypes in these patients.

摘要

目的

本研究描述了 9 位无亲缘关系的新发 NR4A2 基因突变患者的临床和遗传特征。

方法

除 1 例外,所有患者均通过三体外显子组测序确定了变异,并确认了其新生起源。对一个变体进行了靶向 RNA 测序,以确认其剪接效应。通过 GeneMatcher 共享独立发现。

结果

在 8 个无亲缘关系的家庭的患者中发现了 NR4A2 的错义变异和功能丧失变异。1 例患者携带更大的缺失,包括相邻基因。这些病例表现为发育迟缓、低张力(6 例)和癫痫(6 例)。确认了 8 名患者的新生状态。一种变体被证明会影响剪接,导致异常转录本的表达,这些异常转录本可能受到无意义介导的衰变的影响。

结论

本研究强调了 NR4A2 作为神经发育障碍和癫痫疾病基因的重要性。鉴定出的变异很可能导致这些患者的癫痫发作和其他发育表型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26ef/7394879/4e220933f613/41436_2020_815_Fig1_HTML.jpg

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