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Notch 靶基因在嗅感觉神经元多样化过程中的染色质修饰。

Chromatin modification of Notch targets in olfactory receptor neuron diversification.

机构信息

Institute of Molecular and Cellular Biosciences, The University of Tokyo, Bunkyo-ku, Tokyo, Japan.

出版信息

Nat Neurosci. 2011 Dec 25;15(2):224-33. doi: 10.1038/nn.2998.

Abstract

Neuronal-class diversification is central during neurogenesis. This requirement is exemplified in the olfactory system, which utilizes a large array of olfactory receptor neuron (ORN) classes. We discovered an epigenetic mechanism in which neuron diversity is maximized via locus-specific chromatin modifications that generate context-dependent responses from a single, generally used intracellular signal. Each ORN in Drosophila acquires one of three basic identities defined by the compound outcome of three iterated Notch signaling events during neurogenesis. Hamlet, the Drosophila Evi1 and Prdm16 proto-oncogene homolog, modifies cellular responses to these iteratively used Notch signals in a context-dependent manner, and controls odorant receptor gene choice and ORN axon targeting specificity. In nascent ORNs, Hamlet erases the Notch state inherited from the parental cell, enabling a modified response in a subsequent round of Notch signaling. Hamlet directs locus-specific modifications of histone methylation and histone density and controls accessibility of the DNA-binding protein Suppressor of Hairless at the Notch target promoter.

摘要

神经元类别的多样化是神经发生过程中的核心。嗅觉系统就是一个很好的例子,它利用了大量的嗅觉受体神经元 (ORN) 类别。我们发现了一种表观遗传机制,通过特定基因座的染色质修饰,最大限度地增加神经元的多样性,从而产生单一的、通常用于细胞内信号的上下文相关反应。果蝇中的每个 ORN 通过神经发生过程中三个迭代 Notch 信号事件的复合结果获得三种基本身份之一来定义。果蝇 Evi1 和 Prdm16 原癌基因同源物 Hamlet 以依赖上下文的方式修饰细胞对这些迭代使用的 Notch 信号的反应,并控制气味受体基因选择和 ORN 轴突靶向特异性。在新生的 ORN 中,Hamlet 擦除了来自母细胞的 Notch 状态,从而使随后的 Notch 信号传递中产生了修饰后的反应。Hamlet 指导组蛋白甲基化和组蛋白密度的特定基因座修饰,并控制 DNA 结合蛋白 Suppressor of Hairless 在 Notch 靶启动子上的可及性。

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