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Translational research: Rett syndrome and tuberous sclerosis complex.

机译:转化研究:Rett综合征和结节性硬化症。

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PURPOSE OF REVIEW: Rare genetic diseases that affect behavior and cognition provide a unique opportunity to study the mechanisms of neurodevelopmental disorders through the examination of animal models, which can lead to development of hypotheses and treatments testable in human beings. Rett syndrome (RTT) and tuberous sclerosis complex (TSC) are both Mendelian disorders that present with autism, epilepsy, and intellectual disability, in which animal model work has been directly translated into clinical treatment trials currently underway. Here, we review the recent advances in our understanding of RTT and TSC pathogenesis and signaling pathways that may be targeted for novel treatments. RECENT FINDINGS: Animal models generated by engineering mutant forms of the mouse homologs of human genes involved in RTT and TSC have allowed dissection of the molecular pathology. They have further acted as in-vivo assays of potential therapeutic strategies that have translated to human clinical trials. SUMMARY: Single-gene disorders associated with neurodevelopmental disorders provide powerful model systems to study the roles of individual molecules and associated signaling pathways in the genesis of autism, epilepsy, cognitive impairment, and neuropsychiatric symptoms. These diseases are leading to disease-modifying human therapies that may eventually translate to wider therapeutic strategies for autism.
机译:审查的目的:影响行为和认知的罕见遗传疾病为通过检查动物模型来研究神经发育障碍的机制提供了独特的机会,这可能导致假说和可在人类测试的治疗方法的发展。 Rett综合征(RTT)和结节性硬化症(TSC)都是自闭症,癫痫和智力残疾的孟德尔疾病,其中动物模型的工作已直接转化为目前正在进行的临床治疗试验。在这里,我们回顾了我们对RTT和TSC发病机理以及可能针对新型治疗的信号通路的了解的最新进展。最近的发现:通过工程化涉及RTT和TSC的人类基因的小鼠同源物的突变体形式而生成的动物模型已经使分子病理学得以解剖。他们进一步充当了潜在治疗策略的体内分析方法,已转化为人类临床试验。摘要:与神经发育障碍相关的单基因疾病提供了强大的模型系统,以研究自闭症,癫痫,认知障碍和神经精神病学症状中个体分子和相关信号通路的作用。这些疾病正在导致疾病改良型人类疗法,最终可能转化为自闭症的更广泛治疗策略。

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