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DEPDC5 as a potential therapeutic target for epilepsy

机译:DEPDC5作为癫痫的潜在治疗靶标

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Introduction: Dishevelled, Egl-10 and Pleckstrin (DEP) domain-containing protein 5 (DEPDC5) is a protein subunit of the GTPase-activating proteins towards Rags 1 (GATOR1) complex. GATOR1 is a recently identified modulator of mechanistic target of rapamycin (mTOR) activity. mTOR is a key regulator of cell proliferation and metabolism; disruption of the mTOR pathway is implicated in focal epilepsy, both acquired and genetic. Tuberous sclerosis is the prototypic mTOR genetic syndrome with epilepsy, however GATOR1 gene mutations have recently been shown to cause lesional and non-lesional focal epilepsy.Areas covered: This review summarizes the mTOR pathway, including regulators and downstream effectors, emphasizing recent developments in the understanding of the complex role of the GATOR1 complex. We review the epilepsy types associated with mTOR overactivity, including tuberous sclerosis, polyhydramnios megalencephaly symptomatic epilepsy, cortical dysplasia, non-lesional focal epilepsy and post-traumatic epilepsy. Currently available mTOR inhibitors are discussed, primarily rapamycin analogs and ATP competitive mTOR inhibitors.Expert opinion: DEPDC5 is an attractive therapeutic target in focal epilepsy, as effects of DEPDC5 agonists would likely be anti-epileptogenic and more selective than currently available mTOR inhibitors. Therapeutic effects might be synergistic with certain existing dietary therapies, including the ketogenic diet.
机译:介绍:折叠,EGL-10和Pleckstrin(Dep)含域蛋白5(DepdC5)是GTP酶活化蛋白的蛋白质亚基朝向RAG1(Gator1)复合物。 Gator1是最近识别的雷帕霉素(mTOR)活性的机械靶标调节剂。 MTOR是细胞增殖和新陈代谢的关键调节因子; MTOR途径的破坏涉及局灶性癫痫,包括获得和遗传。结核硬化是癫痫原型MTOR遗传综合征,然而,最近已被证明Gator1基因突变导致损伤和非损害局灶性癫痫患者涵盖:本综述总结了MTOR途径,包括监管机构和下游效果,强调最近的发展了解Gator1复杂的复杂作用。我们审查了与MTOR过度育相关的癫痫类型,包括结核硬化症,多羟麦米斯兆畸形症状性癫痫,皮质发育不良,非损害局灶性癫痫和创伤后癫痫症。讨论了目前可用的MTOR抑制剂,主要是雷帕霉素类似物和ATP竞争MTOR抑制剂。普及意见:DEPDC5是局灶性癫痫中有吸引力的治疗靶标,因为DEPDC5激动剂的效果可能是目前可用的MTOR抑制剂的抗癫痫型和更具选择性。治疗效果可能是具有某些现有膳食疗法的协同作用,包括酮饮食。

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