一个中国婴幼儿癫痫家族中新型无义 PPP1R12A 变体的功能分析

IF 2.1 4区 医学 Q3 GENETICS & HEREDITY BMC Medical Genomics Pub Date : 2024-09-27 DOI:10.1186/s12920-024-02009-z
Ling Tong, Xinxin Wang, Huiqin Wang, Rong Yang, Xiaoyan Li, Xiaoguang Yin
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引用次数: 0

摘要

背景:PPP1R12A 缺陷可导致泌尿生殖系统和/或脑畸形综合征(GUBS)。GUBS 主要表现为神经系统或泌尿生殖系统异常,但也有少数病例与新生儿癫痫发作有关。在此,我们报告了一例因 PPP1R12A 的新型变异而导致新生儿癫痫发作的女性新生儿,旨在加强与早期癫痫相关遗传因素的临床和变异数据:方法:采用全外显子组测序和桑格测序对家族变异进行评估,并利用生物信息学对变异进行注释。利用分子动力学(MD)模拟了突变体蛋白质的结构模型,并分析了PPP1R12A和PPP1CB之间的自由结合能。构建了突变体质粒,并利用Western印迹(WB)分析了突变体蛋白的表达,还利用共免疫沉淀(Co-IP)实验分析了突变体蛋白与PPP1CB蛋白之间的相互作用:患者在出生后第二天出现强直阵挛发作。基因检测显示,PPP1R12A 存在杂合变异,即 NM_002480.3:c.2533 C > T (p.Arg845Ter)。父母的基因都是野生型。MD 显示,突变体蛋白质 C 端结构的缺失改变了其结构稳定性,增加了与 PPP1CB 的结合能,表明蛋白质与蛋白质之间的相互作用不稳定。在 WB 上观察到一条低分子量条带,表明该蛋白被截短。Co-IP 表明突变体蛋白不再与 PPP1CB 相互作用,这表明肌球蛋白相复合物的结构稳定性受到了影响:结论:PPP1R12A c.2533 C > T 变异可能是本病例中新生儿癫痫发作的原因。本研究的发现扩大了 PPP1R12A 变异的范围,并强调了截短蛋白在 GUBS 发病机制中的潜在意义。
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Functional analysis of a novel nonsense PPP1R12A variant in a Chinese family with infantile epilepsy.

Background: Defects in PPP1R12A can lead to genitourinary and/or brain malformation syndrome (GUBS). GUBS is primarily characterized by neurological or genitourinary system abnormalities, but a few reported cases are associated with neonatal seizures. Here, we report a case of a female newborn with neonatal seizures caused by a novel variant in PPP1R12A, aiming to enhance the clinical and variant data of genetic factors related to epilepsy in early life.

Methods: Whole-exome and Sanger sequencing were used for familial variant assessment, and bioinformatics was employed to annotate the variant. A structural model of the mutant protein was simulated using molecular dynamics (MD), and the free binding energy between PPP1R12A and PPP1CB was analyzed. A mutant plasmid was constructed, and mutant protein expression was analyzed using western blotting (WB), and the interaction between the mutant and PPP1CB proteins using co-immunoprecipitation (Co-IP) experiments.

Results: The patient experienced tonic-clonic seizures on the second day after birth. Genetic testing revealed a heterozygous variant in PPP1R12A, NM_002480.3:c.2533 C > T (p.Arg845Ter). Both parents had the wild-type gene. MD suggested that loss of the C-terminal structure in the mutant protein altered its structural stability and increased the binding energy with PPP1CB, indicating unstable protein-protein interactions. On WB, a low-molecular-weight band was observed, indicating that the protein was truncated. Co-IP indicated that the mutant protein no longer interacted with PPP1CB, indicating an effect on the structural stability of the myosin phase complex.

Conclusion: The PPP1R12A c.2533 C > T variant may explain the neonatal seizures in the present case. The findings of this study expand the spectrum of PPP1R12A variants and highlight the potential significance of truncated proteins in the pathogenesis of GUBS.

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来源期刊
BMC Medical Genomics
BMC Medical Genomics 医学-遗传学
CiteScore
3.90
自引率
0.00%
发文量
243
审稿时长
3.5 months
期刊介绍: BMC Medical Genomics is an open access journal publishing original peer-reviewed research articles in all aspects of functional genomics, genome structure, genome-scale population genetics, epigenomics, proteomics, systems analysis, and pharmacogenomics in relation to human health and disease.
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