神经炎症
炎症
神经退行性变
全身炎症
脂质体
神经保护
海马结构
代谢组学
生物
海马体
神经科学
脂类学
免疫学
医学
疾病
生物信息学
内科学
作者
Elena Puris,Štěpán Kouřil,Lukáš Najdekr,Seppo Auriola,Sanna Loppi,Paula Korhonen,Mireia Gómez-Budia,Gert Fricker,Katja M. Kanninen,Tarja Malm,David Friedecký,Mikko Gynther
出处
期刊:Neuroscience
[Elsevier]
日期:2022-08-01
卷期号:496: 165-178
被引量:12
标识
DOI:10.1016/j.neuroscience.2022.05.030
摘要
Neuroinflammation is an important feature in the pathogenesis and progression of central nervous system (CNS) diseases including Alzheimer's disease (AD). One of the widely used animal models of peripherally induced neuroinflammation and neurodegeneration is a lipopolysaccharide (LPS)-induced inflammation mouse model. An acute LPS administration has been widely used for investigation of inflammation-associated disease and testing inflammation-targeting drug candidates. In the present metabolomic, lipidomic and proteomic study, we investigated short-term effects of systemic inflammation induced by LPS administration on the mouse plasma and brain cortical and hippocampal metabolome, lipidome as well as expression of the brain cortical proteins which were shown to be involved in inflammation-associated CNS diseases. From a global perspective, the hippocampus was more vulnerable to the effects of LPS-induced systemic inflammation than the cortex. In addition, the study revealed several brain region-specific changes in metabolic pathways and lipids, such as statistically significant increase in several cortical and hippocampal phosphatidylcholines/phosphatidylethanolamines, and significantly decreased levels of brain cortical betaine after LPS treatment in mice. Moreover, LPS treatment in mice caused significantly increased protein expression of GluN1 receptor in the brain cortex. The revealed perturbations in the LPS-induced inflammation mouse model may give insight into the mechanisms underlying inflammation-associated CNS diseases. In addition, the finding of the study provide important information about the appropriate use of the model during target validation and drug candidate testing.
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