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利用 CalEx 小鼠减弱局部和中枢神经系统星形胶质细胞内钙信号

Local and CNS-Wide Astrocyte Intracellular Calcium Signaling Attenuation with CalEx Mice.

机构信息

Department of Physiology

Department of Molecular and Integrative Physiology, Beckman Institute, University of Illinois at Urbana-Champaign, Urbana, Illinois 61801-3704.

出版信息

J Neurosci. 2021 May 26;41(21):4556-4574. doi: 10.1523/JNEUROSCI.0085-21.2021. Epub 2021 Apr 26.

Abstract

Astrocytes exist throughout the CNS and affect neural circuits and behavior through intracellular Ca signaling. Studying the function(s) of astrocyte Ca signaling has proven difficult because of the paucity of tools to achieve selective attenuation. Based on recent studies, we generated and used male and female knock-in mice for Cre-dependent expression of mCherry-tagged hPMCA2w/b to attenuate astrocyte Ca signaling in genetically defined cells (CalEx mice for lcium trusion). We characterized CalEx mice following local AAV-Cre microinjections into the striatum and found reduced astrocyte Ca signaling (∼90%) accompanied with repetitive self-grooming behavior. We also crossed CalEx mice to astrocyte-specific -Cre/ERT2 mice to achieve inducible global CNS-wide Ca signaling attenuation. Within 6 d of induction in the bigenic mice, we observed significantly altered ambulation in the open field, disrupted motor coordination and gait, and premature lethality. Furthermore, with histologic, imaging, and transcriptomic analyses, we identified cellular and molecular alterations in the cerebellum following mCherry-tagged hPMCA2w/b expression. Our data show that expression of mCherry-tagged hPMCA2w/b with CalEx mice throughout the CNS resulted in substantial attenuation of astrocyte Ca signaling and significant behavioral alterations in adult mice. We interpreted these findings candidly in relation to the ability of CalEx to attenuate astrocyte Ca signaling, with regards to additional mechanistic interpretations of the data, and their relation to past studies that reduced astrocyte Ca signaling throughout the CNS. The data and resources provide complementary ways to interrogate the function(s) of astrocytes in multiple experimental scenarios. Astrocytes represent a significant fraction of all brain cells and tile the entire central nervous system. Unlike neurons, astrocytes lack propagated electrical signals. Instead, astrocytes are proposed to use diverse and dynamic intracellular Ca signals to communicate with other cells. An open question concerns if and how astrocyte Ca signaling regulates behavior in adult mice. We approached this problem by generating a new transgenic mouse line to achieve inducible astrocyte Ca signaling attenuation We report our data with this mouse line and we interpret the findings candidly in relation to past studies and within the framework of different mechanistic interpretations.

摘要

星形胶质细胞存在于中枢神经系统(CNS)的各个部位,通过细胞内钙信号影响神经回路和行为。研究星形胶质细胞钙信号的功能非常困难,因为缺乏选择性衰减的工具。基于最近的研究,我们生成并使用雄性和雌性 knock-in 小鼠,用于 Cre 依赖性表达红色荧光蛋白标记的 hPMCA2w/b,以衰减基因定义细胞中的星形胶质细胞钙信号(钙通透性突变体小鼠,用于钙离子内流)。我们在纹状体局部 AAV-Cre 微注射后对 CalEx 小鼠进行了特征描述,发现星形胶质细胞钙信号减弱(约 90%),同时伴有重复性自我梳理行为。我们还将 CalEx 小鼠与星形胶质细胞特异性 -Cre/ERT2 小鼠杂交,以实现诱导性全中枢神经系统范围的钙信号衰减。在双基因小鼠诱导后 6 天内,我们观察到旷场中明显的运动障碍、运动协调和步态障碍以及过早死亡。此外,通过组织学、成像和转录组分析,我们在小脑中发现了 mCherry 标记的 hPMCA2w/b 表达后的细胞和分子改变。我们的数据表明,在整个中枢神经系统中表达 mCherry 标记的 hPMCA2w/b 会导致星形胶质细胞钙信号的显著衰减,并导致成年小鼠的显著行为改变。我们坦率地解释了这些发现与 CalEx 减弱星形胶质细胞钙信号的能力有关,同时考虑了对数据的其他机制解释,以及它们与以往研究的关系,这些研究在整个中枢神经系统中降低了星形胶质细胞钙信号。这些数据和资源提供了互补的方法,可以在多种实验场景下研究星形胶质细胞的功能。星形胶质细胞是大脑细胞的重要组成部分,遍布中枢神经系统。与神经元不同,星形胶质细胞缺乏传播的电信号。相反,星形胶质细胞被认为使用多种动态的细胞内钙信号与其他细胞进行通讯。一个悬而未决的问题是星形胶质细胞钙信号是否以及如何调节成年小鼠的行为。我们通过生成一种新的转基因小鼠品系来解决这个问题,以实现诱导性星形胶质细胞钙信号衰减。我们报告了这种小鼠品系的研究数据,并坦率地解释了这些发现,与过去的研究有关,并在不同的机制解释框架内。

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