Molecular and genetic insights into an infantile epileptic encephalopathy - CDKL5 disorder.

Frontiers in Biology Pub Date : 2017-02-01 Epub Date: 2017-01-23 DOI:10.1007/s11515-016-1438-7
Ailing Zhou, Song Han, Zhaolan Joe Zhou
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引用次数: 18

Abstract

Background: The discovery that mutations in cyclin-dependent kinase-like 5 (CDKL5) gene are associated with infantile epileptic encephalopathy has stimulated world-wide research effort to understand the molecular and genetic basis of CDKL5 disorder. Given the large number of literature published thus far, this review aims to summarize current genetic studies, draw a consensus on proposed molecular functions, and point to gaps of knowledge in CDKL5 research.

Methods: A systematic review process was conducted using the PubMed search engine focusing on CDKL5 studies in the recent ten years. We analyzed these publications and summarized the findings into four sections: genetic studies, CDKL5 expression patterns, molecular functions, and animal models. We also discussed challenges and future directions in each section.

Results: On the clinical side, CDKL5 disorder is characterized by early onset epileptic seizures, intellectual disability, and stereotypical behaviors. On the research side, a series of molecular and genetic studies in human patients, cell cultures and animal models have established the causality of CDKL5 to the infantile epileptic encephalopathy, and pointed to a key role for CDKL5 in regulating neuronal function in the brain. Mouse models of CDKL5 disorder have also been developed, and notably, manifest behavioral phenotypes, mimicking numerous clinical symptoms of CDKL5 disorder and advancing CDKL5 research to the preclinical stage.

Conclusions: Given what we have learned thus far, future identification of robust, quantitative, and sensitive outcome measures would be the key in animal model studies, particularly in heterozygous females. In the meantime, molecular and cellular studies of CDKL5 should focus on mechanism-based investigation and aim to uncover druggable targets that offer the potential to rescue or ameliorate CDKL5 disorder-related phenotypes.

婴儿癫痫性脑病- CDKL5紊乱的分子和遗传学见解。
背景:周期蛋白依赖性激酶样5 (CDKL5)基因突变与婴儿癫痫性脑病相关的发现,刺激了全球范围内对CDKL5疾病分子和遗传基础的研究。鉴于迄今为止发表的大量文献,本综述旨在总结当前的遗传学研究,对所提出的分子功能达成共识,并指出CDKL5研究中的知识空白。方法:利用PubMed搜索引擎对近十年来的CDKL5研究进行系统综述。我们分析了这些出版物,并将研究结果归纳为四个部分:遗传学研究、CDKL5表达模式、分子功能和动物模型。我们还在每个部分中讨论了挑战和未来的方向。结果:在临床方面,CDKL5障碍以早发性癫痫发作、智力残疾和刻板行为为特征。在研究方面,一系列对人类患者、细胞培养和动物模型的分子和遗传学研究已经确立了CDKL5与婴儿癫痫性脑病的因果关系,并指出了CDKL5在调节大脑神经元功能方面的关键作用。CDKL5疾病的小鼠模型也被开发出来,值得注意的是,表现出行为表型,模仿了CDKL5疾病的许多临床症状,并将CDKL5研究推进到临床前阶段。结论:鉴于我们目前所了解到的,未来确定可靠、定量和敏感的结果测量将是动物模型研究的关键,特别是在杂合雌性中。与此同时,CDKL5的分子和细胞研究应侧重于基于机制的研究,并旨在发现有可能拯救或改善CDKL5疾病相关表型的可药物靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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期刊介绍: Frontiers in Biology is a journal in the field of biology, covering areas including microbiology, cell biology, biochemistry and molecular biology, developmental biology, genetics, paleontology, botany, zoology, aquatic biology, conservation biology, ecology and other related disciplines.
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