Milatovic Dejan, Zaja-Milatovic Snjezana, Montine Kathleen S, Shie Feng-Shiun, Montine Thomas J
J Neuroinflammation. 2004 Oct 21;1(1):20. doi: 10.1186/1742-2094-1-20.
The cause-and-effect relationship between innate immune activation and neurodegeneration has been difficult to prove in complex animal models and patients. Here we review findings from a model of direct innate immune activation via CD14 stimulation using intracerebroventricular injection of lipopolysaccharide. These data show that CD14-dependent innate immune activation in cerebrum leads to the closely linked outcomes of neuronal membrane oxidative damage and dendritic degeneration. Both forms of neuronal damage could be blocked by ibuprofen and alpha-tocopherol, but not naproxen or gamma-tocopherol, at pharmacologically relevant concentrations. This model provides a convenient method to determine effective agents and their appropriate dose ranges for protecting neurons from CD14-activated innate immunity-mediated damage, and can guide drug development for diseases, such as Alzheimer disease, that are thought to derive in part from CD14-activated innate immune response.
在复杂的动物模型和患者中,先天免疫激活与神经退行性变之间的因果关系一直难以证实。在此,我们回顾了通过脑室内注射脂多糖直接激活先天免疫的模型所获得的研究结果。这些数据表明,大脑中依赖CD14的先天免疫激活会导致神经元膜氧化损伤和树突退化这两个紧密相关的结果。在药理学相关浓度下,布洛芬和α-生育酚可阻断这两种形式的神经元损伤,但萘普生或γ-生育酚则不能。该模型提供了一种便捷的方法,用于确定保护神经元免受CD14激活的先天免疫介导损伤的有效药物及其合适的剂量范围,并可指导针对诸如阿尔茨海默病等部分被认为源于CD14激活的先天免疫反应的疾病的药物开发。
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