Lee Wonil, Moon Minho, Kim Hyo Geun, Lee Tae Hee, Oh Myung Sook
Department of Life and Nanopharmaceutical Science, Graduate School and Kyung Hee East-West Pharmaceutical Research Institute, Kyung Hee University, 26 Kyungheedae-ro, Dongdaemun-gu, Seoul, 130-701, Republic of Korea.
Molecular Neurobiology Laboratory, McLean Hospital/Harvard Medical School, Belmont, MA, 02478, USA.
J Neuroinflammation. 2015 May 23;12:102. doi: 10.1186/s12974-015-0324-6.
Heat stress induces many pathophysiological responses and has a profound impact on brain structure. It has been demonstrated that exposure to high temperature induces cognitive impairment in experimental animals and humans. Although the effects of heat stress have long been studied, the mechanisms by which heat stress affects brain structure and cognition not well understood.
In our longitudinal study of mice exposed to heat over 7, 14, or 42 days, we found that heat stress time dependently impaired cognitive function as determined by Y-maze, passive avoidance, and novel object recognition tests. To elucidate the histological mechanism by which thermal stress inhibited cognitive abilities, we examined heat stress-induced inflammation in the hippocampus.
In mice subjected to heat exposure, we found: 1) an increased number of glial fibrillary acid protein (GFAP)- and macrophage-1 antigen (Mac-1)-positive cells, 2) up-regulated nuclear factor (NF)-κB, a master regulator of inflammation, and 3) marked increases in cyclooxygenase-2 (COX-2), inducible nitric oxide synthase (iNOS), and cytokine interleukin (IL)-1β and tumor necrosis factor (TNF)-α in the mouse hippocampus. We also observed that neuronal and synaptic densities were degenerated significantly in hippocampal regions after heat exposure, as determined by histological analysis of neuronal nuclei (NeuN), postsynaptic density protein 95 (PSD-95), and synaptophysin expression. Moreover, in heat-exposed mice, we found that the number of cells positive for doublecortin (DCX), a marker of neurogenesis, was significantly decreased compared with control mice. Finally, anti-inflammatory agent minocycline inhibited the heat stress-induced cognitive deficits and astogliosis in mice.
Together, these findings suggest that heat stress can lead to activation of glial cells and induction of inflammatory molecules in the hippocampus, which may act as causative factors for memory loss, neuronal death, and impaired adult neurogenesis.
热应激会引发多种病理生理反应,并对脑结构产生深远影响。已有研究表明,暴露于高温环境会导致实验动物和人类出现认知障碍。尽管长期以来一直在研究热应激的影响,但其影响脑结构和认知的机制尚未完全明确。
在我们对小鼠进行7天、14天或42天热暴露的纵向研究中,我们发现热应激会随时间推移损害认知功能,这通过Y迷宫、被动回避和新物体识别测试得以确定。为阐明热应激抑制认知能力的组织学机制,我们检测了热应激诱导的海马体炎症反应。
在热暴露的小鼠中,我们发现:1)胶质纤维酸性蛋白(GFAP)和巨噬细胞-1抗原(Mac-1)阳性细胞数量增加;2)炎症的主要调节因子核因子(NF)-κB上调;3)小鼠海马体中环氧合酶-2(COX-2)、诱导型一氧化氮合酶(iNOS)、细胞因子白细胞介素(IL)-1β和肿瘤坏死因子(TNF)-α显著增加。通过对神经元细胞核(NeuN)、突触后密度蛋白95(PSD-95)和突触素表达的组织学分析,我们还观察到热暴露后海马区的神经元和突触密度显著退化。此外,在热暴露的小鼠中,我们发现与对照小鼠相比,双皮质素(DCX,一种神经发生标志物)阳性细胞数量显著减少。最后,抗炎药物米诺环素可抑制热应激诱导的小鼠认知缺陷和星形胶质细胞增生。
综上所述,这些发现表明热应激可导致海马体中胶质细胞活化和炎症分子诱导,这可能是导致记忆丧失、神经元死亡和成年神经发生受损的致病因素。
Zotero 插件
