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在经典条件反射的神经相关物中,ARC 即刻早期基因的特征描述和转录激活。

Characterization and Transcriptional Activation of the Immediate Early Gene ARC During a Neural Correlate of Classical Conditioning.

机构信息

Neuroscience Group, Division of Basic Biomedical Sciences, University of South Dakota Sanford School of Medicine, 414 E. Clark St, Vermillion, SD, 57069, USA.

出版信息

J Mol Neurosci. 2019 Nov;69(3):380-390. doi: 10.1007/s12031-019-01367-z. Epub 2019 Jul 4.

Abstract

Plasticity and learning genes require regulatory mechanisms that have the flexibility to respond to a variety of sensory stimuli to generate adaptive behavioral responses. The immediate early gene (IEG) activity-regulated cytoskeleton-associated protein (ARC) is rapidly induced not only by neuronal stimulation but also during a variety of learning tasks. How ARC is regulated in response to complex stimuli during associative learning remains to be fully detailed. Here, we characterized the structure of the ARC gene in the pond turtle and mechanisms of its transcriptional activation during a neural correlate of eyeblink classical conditioning. The tARC gene is regulated in part by the presence of paused polymerase (RNAPII) that is poised at the promoter for rapid gene induction. Conditioning induces permissive chromatin modifications in the tARC promoter that allows binding by the transcription factor cAMP response element-binding protein (CREB) within 5 min of training. During learning acquisition, the pausing factor negative elongation factor (NELF) dissociates from the promoter thereby releasing RNAPII for active transcription. Data additionally suggest that the DNA insulator protein CCCTC-binding factor (CTCF) is required for transcription by mediating a learning-induced interaction of the ARC promoter with an enhancer element. Our study suggests that the learning-inducible IEG tARC utilizes both paused RNAPII and rapid chromatin modifications that allow for dynamic gene responsiveness required when an organism is presented with a variety of environmental stimuli.

摘要

可塑性和学习基因需要具有灵活性的调节机制,以响应各种感觉刺激,从而产生适应性的行为反应。活性调节细胞骨架相关蛋白(ARC)作为即刻早期基因(IEG),不仅可以被神经元刺激诱导,还可以在各种学习任务中被诱导。ARC 如何响应复杂刺激并在联想学习中被调控,仍有待进一步详细研究。本研究在池塘龟中对 ARC 基因结构进行了特征描述,并阐明了其在眨眼经典条件反射神经相关中的转录激活机制。tARC 基因的部分表达受到暂停聚合酶(RNAPII)的调控,RNAPII 暂停在启动子处,以便快速诱导基因表达。条件作用会引起 tARC 启动子中允许转录因子 cAMP 反应元件结合蛋白(CREB)结合的许可性染色质修饰,该修饰在训练后 5 分钟内发生。在学习获得过程中,暂停因子负延伸因子(NELF)从启动子解离,从而释放 RNAPII 以进行活跃转录。此外,数据表明,CCCTC 结合因子(CTCF)作为 DNA 绝缘子蛋白,通过介导学习诱导的 ARC 启动子与增强子元件之间的相互作用,对转录是必需的。本研究表明,学习诱导的 IEG tARC 既利用了暂停的 RNAPII,也利用了快速的染色质修饰,这使得生物体在面对各种环境刺激时,能够产生动态的基因响应能力。

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