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Chemogenomic analysis reveals key role for lysine acetylation in regulating Arc stability

机译:化学基因组分析揭示了赖氨酸乙酰化在调节电弧稳定性中的关键作用

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The role of Arc in synaptic plasticity and memory consolidation has been investigated for many years with recent evidence that defects in the expression or activity of this immediate-early gene may also contribute to the pathophysiology of brain disorders including schizophrenia and fragile X syndrome. These results bring forward the concept that reversing Arc abnormalities could provide an avenue to improve cognitive or neurological impairments in different disease contexts, but how to achieve this therapeutic objective has remained elusive. Here, we present results from a chemogenomic screen that probed a mechanistically diverse library of small molecules for modulators of BDNF-induced Arc expression in primary cortical neurons. This effort identified compounds with a range of influences on Arc, including promoting its acetylation—a previously uncharacterized post-translational modification of this protein. Together, our data provide insights into the control of Arc that could be targeted to harness neuroplasticity for clinical applications.
机译:多年来,一直在研究Arc在突触可塑性和记忆巩固中的作用,最近的证据表明,该即早基因的表达或活性缺陷也可能导致包括精神分裂症和脆性X综合征在内的脑部疾病的病理生理。这些结果提出了一个概念,即逆转电弧异常可以为改善不同疾病背景下的认知或神经功能障碍提供途径,但是如何实现该治疗目标仍然​​是未知的。在这里,我们提出了从化学基因组学筛选的结果,该筛选探索了机制多样的小分子文库,用于调控BDNF诱导的原代皮层神经元Arc表达。这项工作确定了对Arc有多种影响的化合物,包括促进其乙酰化-这种蛋白质以前未表征的翻译后修饰。在一起,我们的数据提供了对弧控制的见解,可以针对利用神经可塑性进行临床应用。

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