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解析 CASK:与男性 MICPCH 表型相关的新型剪接位点变异。

Dissecting CASK: Novel splice site variant associated with male MICPCH phenotype.

机构信息

Department of Medical Genetics, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Alberta, Canada.

Alberta Health Services, Edmonton Zone, Alberta, Canada.

出版信息

Clin Genet. 2024 Dec;106(6):764-768. doi: 10.1111/cge.14610. Epub 2024 Aug 30.

Abstract

CASK (MIM#300172), encoding a calcium/calmodulin-dependent serine protein kinase, is crucial for synaptic transmission and gene regulation during neural development. Pathogenic variants of CASK are known to cause several neurodevelopmental disorders, including X-linked intellectual disability and microcephaly with pontine and cerebellar hypoplasia (MICPCH). This study introduces a novel, de novo synonymous CASK variant (NM_001367721.1: c.1737G>A, p.(Glu579=)), discovered in a male patient diagnosed with MICPCH, characterized by microcephaly, developmental delay, visual impairment, and myoclonic seizures. The variant disrupts a donor splice-site at the end of exon 18. Transcriptomic analysis of blood identified 12 different CASK transcripts secondary to the synonymous variant. Nearly one third of these transcripts were predicted to result in nonsense mediated decay or protein degradation. Protein modeling revealed structural alterations in the PDZ functional domain of CASK, due to exon 18 deletion. Our findings highlight the utility of transcriptomic analysis in demonstrating the underlying disease mechanism in neurodevelopmental disorders.

摘要

CASK(MIM#300172),编码钙/钙调蛋白依赖性丝氨酸蛋白激酶,对于神经发育过程中的突触传递和基因调控至关重要。已知 CASK 的致病变体可导致多种神经发育障碍,包括 X 连锁智力障碍和伴有桥脑和小脑发育不良的小头畸形(MICPCH)。本研究介绍了一种新的、从头的同义 CASK 变体(NM_001367721.1:c.1737G>A,p.(Glu579=)),该变体在一名被诊断为 MICPCH 的男性患者中发现,其特征是小头畸形、发育迟缓、视力障碍和肌阵挛性癫痫发作。该变体破坏了外显子 18 末端的供体位点剪接。血液转录组分析鉴定出 12 种不同的 CASK 转录本,这些转录本是由于同义变体引起的。这些转录本中近三分之一被预测会导致无意义介导的衰变或蛋白降解。蛋白质建模显示,由于外显子 18 缺失,CASK 的 PDZ 功能域发生了结构改变。我们的研究结果强调了转录组分析在展示神经发育障碍中潜在疾病机制的应用。

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