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突触调节。

Synapse Regulation.

机构信息

Division of Medical Sciences, University of Victoria, Victoria, BC, Canada.

Division of Psychiatry Research, University of Zurich, Schlieren, Switzerland.

出版信息

Adv Neurobiol. 2024;37:179-208. doi: 10.1007/978-3-031-55529-9_11.

Abstract

Microglia are the resident immune cells of the brain. As such, they rapidly detect changes in normal brain homeostasis and accurately respond by fine-tuning in a tightly regulated manner their morphology, gene expression, and functional behavior. Depending on the nature of these changes, microglia can thicken and retract their processes, proliferate and migrate, release numerous signaling factors and compounds influencing neuronal physiology (e.g., cytokines and trophic factors), in addition to secreting proteases able to transform the extracellular matrix, and phagocytosing various types of cellular debris, etc. Because microglia also transform rapidly (on a time scale of minutes) during experimental procedures, studying these very special cells requires methods that are specifically non-invasive. The development of such methods has provided unprecedented insights into the roles of microglia during normal physiological conditions. In particular, transcranial two-photon in vivo imaging revealed that presumably "resting" microglia continuously survey the brain parenchyma with their highly motile processes, in addition to modulating their structural and functional interactions with neuronal circuits along the changes in neuronal activity and behavioral experience occurring throughout the lifespan. In this chapter, we will describe how surveillant microglia interact with synaptic elements and modulate the number, maturation, function, and plasticity of synapses in the healthy developing, mature, and aging brain, with consequences on neuronal activity, learning and memory, and the behavioral outcome.

摘要

小胶质细胞是大脑的固有免疫细胞。因此,它们能迅速检测到正常大脑内环境平衡的变化,并通过精细调节其形态、基因表达和功能行为来准确响应。根据这些变化的性质,小胶质细胞可以增粗和缩回其突起,增殖和迁移,释放影响神经元生理的多种信号因子和化合物(例如细胞因子和营养因子),此外还分泌能够改变细胞外基质的蛋白酶,并吞噬各种类型的细胞碎片等。由于小胶质细胞在实验过程中也会迅速(在几分钟的时间尺度上)发生转变,因此研究这些非常特殊的细胞需要专门的非侵入性方法。这些方法的发展为理解小胶质细胞在正常生理条件下的作用提供了前所未有的见解。特别是,颅穿透双光子在体成像揭示了推测为“静止”的小胶质细胞通过其高度运动的突起不断监测脑实质,此外还调节其与神经元回路的结构和功能相互作用,以适应整个生命周期中神经元活动和行为经验的变化。在本章中,我们将描述监视小胶质细胞如何与突触元件相互作用,并调节健康发育、成熟和衰老大脑中突触的数量、成熟度、功能和可塑性,从而影响神经元活动、学习和记忆以及行为结果。

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