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复杂染色体重排导致的全 FGF12 基因重复与 West 综合征相关。

Entire FGF12 duplication by complex chromosomal rearrangements associated with West syndrome.

机构信息

Department of Pediatrics, Chigasaki Municipal Hospital, Chigasaki, Japan.

Department of Human Genetics, Yokohama City University Graduate School of Medicine, Yokohama, Japan.

出版信息

J Hum Genet. 2019 Oct;64(10):1005-1014. doi: 10.1038/s10038-019-0641-1. Epub 2019 Jul 16.

Abstract

Complex rearrangements of chromosomes 3 and 9 were found in a patient presenting with severe epilepsy, developmental delay, dysmorphic facial features, and skeletal abnormalities. Molecular cytogenetic analysis revealed 46,XX.ish der(9)(3qter→3q28::9p21.1→9p22.3::9p22.3→9qter)(RP11-368G14+,RP11-299O8-,RP11-905L2++,RP11-775E6++). Her dysmorphic features are consistent with 3q29 microduplication syndrome and inv dup del(9p). Trio-based WES of the patient revealed no pathogenic single nucleotide variants causing epilepsy, but confirmed a 3q28q29 duplication involving FGF12, which encodes fibroblast growth factor 12. FGF12 positively regulates the activity of voltage-gated sodium channels. Recently, only one recurrent gain-of-function variant [NM_021032.4:c.341G>A:p.(Arg114His)] in FGF12 was found in a total of 10 patients with severe early-onset epilepsy. We propose that the patient's entire FGF12 duplication may be analogous to the gain-of-function variant in FGF12 in the epileptic phenotype of this patient.

摘要

患者表现为严重癫痫、发育迟缓、面部畸形特征和骨骼异常,我们发现其存在染色体 3 和 9 的复杂重排。分子细胞遗传学分析显示其核型为 46,XX.ish der(9)(3qter→3q28::9p21.1→9p22.3::9p22.3→9qter)(RP11-368G14+,RP11-299O8-,RP11-905L2++,RP11-775E6++)。其面部畸形特征与 3q29 微重复综合征和 inv dup del(9p)一致。对该患者进行基于三核苷酸的 WES 检测未发现导致癫痫的致病性单核苷酸变异,但证实了 FGF12 所在的 3q28q29 重复,该基因编码成纤维细胞生长因子 12。FGF12 可正向调节电压门控钠离子通道的活性。最近,在总共 10 名患有严重早发性癫痫的患者中仅发现了 FGF12 中一个重复获得功能的变异 [NM_021032.4:c.341G>A:p.(Arg114His)]。我们推测,该患者的 FGF12 整个重复可能类似于 FGF12 获得功能变异在该患者癫痫表型中的作用。

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