Literature DB >> 34128226

Microglia proliferation plays distinct roles in acquired epilepsy depending on disease stages.

Martina Di Nunzio1, Rossella Di Sapia1, Diletta Sorrentino1, Valentina Kebede1, Milica Cerovic1, Giorgia S Gullotta2, Marco Bacigaluppi2, Etienne Audinat3, Nicola Marchi3, Teresa Ravizza1, Annamaria Vezzani1.   

Abstract

OBJECTIVE: Microgliosis occurs in animal models of acquired epilepsy and in patients. It includes cell proliferation that is associated with seizure frequency and decreased neuronal cells in human epilepsy. The role of microglia proliferation in the development of acquired epilepsy is unknown; thus, we examined its contribution to spontaneous seizure, neurodegeneration, and cognitive deficits in different disease phases.
METHODS: We used a model of acquired epilepsy triggered by intra-amygdala kainic acid in C57BL6N adult male mice. Mice were electroencephalographically (EEG) monitored (24/7) during status epilepticus and in early and chronic disease. Microglia proliferation was blocked by GW2580, a selective CSF1 receptor inhibitor, supplemented in the diet for 21 days from status epilepticus onset. Then, mice were returned to placebo diet until experiment completion. Control mice were exposed to status epilepticus and fed with placebo diet. Experimental mice were tested in the novel object recognition test (NORT) and in Barnes maze, and compared to control and sham mice. At the end of the behavioral test, mice were killed for brain histopathological analysis. Additionally, seizure baseline was monitored in chronic epileptic mice, then mice were fed for 14 days with GW2580 or placebo diet under 24/7 EEG recording.
RESULTS: GW2580 prevented microglia proliferation in mice undergoing epilepsy, whereas it did not affect microglia or basal excitatory neurotransmission in the hippocampus of naive mice. Mice with occluded microglia proliferation during early disease development underwent status epilepticus and subsequent epilepsy similar to placebo diet mice, and were similarly impaired in NORT, with improvement in Barnes maze. GW2580-treated mice displayed neuroprotection in the hippocampus. In contrast, blockade of microglia proliferation in chronic epileptic mice resulted in spontaneous seizure reduction versus placebo mice. SIGNIFICANCE: Microglia proliferation during early disease contributes to neurodegeneration, whereas in late chronic disease it contributes to seizures. Timely pharmacological interference with microglia proliferation may offer a potential target for improving disease outcomes.
© 2021 International League Against Epilepsy.

Entities:  

Keywords:  CSF1 receptor; epileptogenesis; microglia proliferation; neuroprotection

Mesh:

Substances:

Year:  2021        PMID: 34128226     DOI: 10.1111/epi.16956

Source DB:  PubMed          Journal:  Epilepsia        ISSN: 0013-9580            Impact factor:   5.864


  5 in total

Review 1.  Mechanisms Involved in Epileptogenesis in Alzheimer's Disease and Their Therapeutic Implications.

Authors:  Miren Altuna; Gonzalo Olmedo-Saura; María Carmona-Iragui; Juan Fortea
Journal:  Int J Mol Sci       Date:  2022-04-13       Impact factor: 6.208

Review 2.  Sleep Disruption Worsens Seizures: Neuroinflammation as a Potential Mechanistic Link.

Authors:  Herlinda Bonilla-Jaime; Helena Zeleke; Asheebo Rojas; Claudia Espinosa-Garcia
Journal:  Int J Mol Sci       Date:  2021-11-20       Impact factor: 5.923

3.  Glial Cell Collaboration in Space and Time Contributes to Epileptogenesis.

Authors:  Nigel C Jones; Idrish Ali
Journal:  Epilepsy Curr       Date:  2021-09-16       Impact factor: 7.500

4.  Conditional knockout of ASK1 in microglia/macrophages attenuates epileptic seizures and long-term neurobehavioural comorbidities by modulating the inflammatory responses of microglia/macrophages.

Authors:  Yiying Zhang; Zhangyang Wang; Rongrong Wang; Lu Xia; Yiying Cai; Fangchao Tong; Yanqin Gao; Jing Ding; Xin Wang
Journal:  J Neuroinflammation       Date:  2022-08-08       Impact factor: 9.587

5.  Reactive morphology of dividing microglia following kainic acid administration.

Authors:  Tabitha R F Green; Sean M Murphy; Maria P Moreno-Montano; Etienne Audinat; Rachel K Rowe
Journal:  Front Neurosci       Date:  2022-09-29       Impact factor: 5.152
  5 in total

北京卡尤迪生物科技股份有限公司 © 2022-2023.