首页> 美国卫生研究院文献>Frontiers in Molecular Neuroscience >The Autism and Angelman Syndrome Protein Ube3A/E6AP: The Gene E3 Ligase Ubiquitination Targets and Neurobiological Functions
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The Autism and Angelman Syndrome Protein Ube3A/E6AP: The Gene E3 Ligase Ubiquitination Targets and Neurobiological Functions

机译:自闭症和安格曼综合症蛋白Ube3A / E6AP:基因E3连接酶泛素化靶标和神经生物学功能。

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摘要

UBE3A is a gene implicated in neurodevelopmental disorders. The protein product of UBE3A is the E3 ligase E6-associated protein (E6AP), and its expression in the brain is uniquely regulated via genetic imprinting. Loss of E6AP expression leads to the development of Angelman syndrome (AS), clinically characterized by lack of speech, abnormal motor development, and the presence of seizures. Conversely, copy number variations (CNVs) that result in the overexpression of E6AP are strongly associated with the development of autism spectrum disorders (ASDs), defined by decreased communication, impaired social interest, and increased repetitive behavior. In this review article, we focus on the neurobiological function of Ube3A/E6AP. As an E3 ligase, many functional target proteins of E6AP have been discovered, including p53, Arc, Ephexin5, and SK2. On a neuronal level, E6AP is widely expressed within the cell, including dendritic arbors, spines, and the nucleus. E6AP regulates neuronal morphological maturation and plays an important role in synaptic plasticity and cortical development. These molecular findings provide insight into our understanding of the molecular events underlying AS and ASDs.
机译:UBE3A是与神经发育障碍有关的基因。 UBE3A的蛋白质产物是E3连接酶E6相关蛋白(E6AP),其在大脑中的表达通过遗传印迹来唯一调控。 E6AP表达的丧失会导致Angelman综合征(AS)的发展,其临床特征是缺乏言语,运动发育异常和癫痫发作。相反,导致E6AP过度表达的拷贝数变异(CNV)与自闭症谱系障碍(ASD)的发展密切相关,自闭症谱系障碍的定义是交流减少,社会兴趣减弱和重复行为增加。在这篇综述文章中,我们重点介绍Ube3A / E6AP的神经生物学功能。作为E3连接酶,已经发现了许多E6AP的功能靶蛋白,包括p53,Arc,Ephexin5和SK2。在神经元水平上,E6AP在细胞内广泛表达,包括树突状乔木,刺和细胞核。 E6AP调节神经元的形态成熟,并在突触可塑性和皮质发育中起重要作用。这些分子发现为我们对AS和ASD潜在分子事件的理解提供了见识。

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