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Meis/UNC-62 亚型依赖性调控 CoupTF-II/UNC-55 以及 GABA 能运动神经元亚型分化。

Meis/UNC-62 isoform dependent regulation of CoupTF-II/UNC-55 and GABAergic motor neuron subtype differentiation.

作者信息

Campbell Richard F, Walthall Walter W

机构信息

Department of Biology, Georgia State University, Atlanta, GA 30303, United States.

Department of Biology, Georgia State University, Atlanta, GA 30303, United States.

出版信息

Dev Biol. 2016 Nov 15;419(2):250-261. doi: 10.1016/j.ydbio.2016.09.009. Epub 2016 Sep 12.

Abstract

Gene regulatory networks orchestrate the assembly of functionally related cells within a cellular network. Subtle differences often exist among functionally related cells within such networks. How differences are created among cells with similar functions has been difficult to determine due to the complexity of both the gene and the cellular networks. In Caenorhabditis elegans, the DD and VD motor neurons compose a cross-inhibitory, GABAergic network that coordinates dorsal and ventral muscle contractions during locomotion. The Pitx2 homologue, UNC-30, acts as a terminal selector gene to create similarities and the Coup-TFII homologue, UNC-55, is necessary for creating differences between the two motor neuron classes. What is the organizing gene regulatory network responsible for initiating the expression of UNC-55 and thus creating differences between the DD and VD motor neurons? We show that the unc-55 promoter has modules that contain Meis/UNC-62 binding sites. These sites can be subdivided into regions that are capable of activating or repressing UNC-55 expression in different motor neurons. Interestingly, different isoforms of UNC-62 are responsible for the activation and the stabilization of unc-55 transcription. Furthermore, specific isoforms of UNC-62 are required for proper synaptic patterning of the VD motor neurons. Isoform specific regulation of differentiating neurons is a relatively unexplored area of research and presents a mechanism for creating differences among functionally related cells within a network.

摘要

基因调控网络精心编排细胞网络中功能相关细胞的组装。在这样的网络中,功能相关的细胞之间常常存在细微差异。由于基因网络和细胞网络的复杂性,功能相似的细胞之间如何产生差异一直难以确定。在秀丽隐杆线虫中,DD和VD运动神经元组成一个交叉抑制的、γ-氨基丁酸能网络,在运动过程中协调背侧和腹侧肌肉收缩。Pitx2同源物UNC-30作为一个终末选择基因来产生相似性,而Coup-TFII同源物UNC-55对于在这两类运动神经元之间产生差异是必需的。启动UNC-55表达从而在DD和VD运动神经元之间产生差异的组织基因调控网络是什么?我们发现unc-55启动子具有包含Meis/UNC-62结合位点的模块。这些位点可细分为能够在不同运动神经元中激活或抑制UNC-55表达的区域。有趣的是,UNC-62的不同异构体负责unc-55转录的激活和稳定。此外,UNC-62的特定异构体是VD运动神经元正确突触模式形成所必需的。异构体对分化神经元的特异性调控是一个相对未被探索的研究领域,它为在网络中功能相关的细胞之间产生差异提供了一种机制。

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