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Long-term environmental enrichment affects microglial morphology in middle age mice

机译:长期环境富集影响中年小鼠的小胶质细胞形态

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摘要

Aging is associated with increased central nervous system inflammation, in large part due to dysfunctional microglia. Environmental enrichment (EE) provides a model for studying the dynamics of lifestyle factors in the development of age-related neuroinflammation and microglial dysfunction. EE results in improvements in learning and memory, metabolism, and mental health in a variety of animal models. We recently reported that implementing EE in middle age promotes healthy aging. In the present study, we investigated whether EE influences microglial morphology, and whether EE is associated with changes in expression of microglial and neuroinflammatory markers. Inflammatory cytokines and MHC-II were reduced following 12-month EE in 10-month-old mice. Long-term EE for 7.5 months resulted in broad increases in Iba1 expression in hippocampus, hypothalamus, and amygdala detected by immunohistochemistry. Quantification of microglial morphology reveal both hypertrophy and ramification in these three brain regions, without increases in microglial cell density. These data indicate that long-term EE implemented in middle age results in a microglial state distinct from that of normal aging in standard laboratory housing, in specific brain regions, associated with reduced neuroinflammatory markers and improvement of systemic metabolism.
机译:衰老与中枢神经系统炎症增加有关,这在很大程度上是由于小胶质细胞功能障碍。环境富集(EE)提供了一个模型,用于研究与年龄相关的神经炎症和小胶质细胞功能障碍发展中的生活方式因素的动态。 EE可以改善各种动物模型的学习和记忆,新陈代谢以及心理健康。我们最近报道说,在中年实施EE可以促进健康的衰老。在本研究中,我们调查了EE是否影响小胶质细胞的形态,以及EE是否与小胶质细胞和神经炎性标志物的表达变化有关。 EE在12个月大的小鼠中,炎症细胞因子和MHC-II减少了。免疫学7.5个月的长期EE导致海马,下丘脑和杏仁核中Iba1表达的广泛增加。小胶质细胞形态的定量显示这三个大脑区域的肥大和分支,而没有小胶质细胞密度的增加。这些数据表明,在中年实施的长期EE会导致小胶质细胞状态不同于正常实验室在特定大脑区域的正常衰老状态,这与减少神经炎性标志物和改善全身代谢有关。

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