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Development of a novel FIJI-based method to investigate neuronal circuitry in neonatal mice

机译:一种新型的基于FIJI的方法研究新生儿小鼠神经元回路的开发

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摘要

The emergence of systems neuroscience tools requires parallel generation of objective analytical workflows for experimental neuropathology. We developed an objective analytical workflow that we used to determine how specific autonomic neural lineages change during postnatal development. While a wealth of knowledge exists regarding postnatal alterations in respiratory neural function, how these neural circuits change and develop in the weeks following birth remains less clear. In this study, we developed our workflow by combining genetic mouse modeling and quantitative immunofluorescent confocal microscopy and used this to examine the postnatal development of neural circuits derived from the transcription factors NKX2.2 and OLIG3 into three medullary respiratory nuclei. Our automated FIJI-based image analysis workflow rapidly and objectively quantified synaptic puncta in user-defined anatomic regions. Using our objective workflow, we found that the density and estimated total number of Nkx2.2-derived afferents into the PreBötzinger Complex significantly decreased with postnatal age during the first three weeks of postnatal life. These data indicate that Nkx2.2-derived structures differentially influence PreBötzinger Complex respiratory oscillations at different stages of postnatal development.
机译:系统神经科学工具的出现要求并行生成用于实验神经病理学的客观分析工作流程。我们开发了一种客观的分析工作流程,用于确定产后发育过程中特定自主神经谱系的变化。尽管关于呼吸道神经功能的产后改变存在着丰富的知识,但是这些神经回路在出生后几周内如何变化和发展仍然不清楚。在这项研究中,我们通过结合遗传小鼠建模和定量免疫荧光共聚焦显微镜开发了我们的工作流程,并将其用于检查源自转录因子NKX2.2和OLIG3进入三个延髓呼吸核的神经回路的产后发育。我们基于FIJI的自动化图像分析工作流程可快速,客观地量化用户定义的解剖区域中的突触点。使用我们的客观工作流程,我们发现,在出生后前三周,随着出生年龄的增长,进入PreBötzinger复合体的Nkx2.2派生的密度和估计总数显着降低。这些数据表明,Nkx2.2衍生的结构在产后发育的不同阶段差异影响PreBötzinger复合体呼吸振荡。

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