Glia activation and its role in oxidative stress

被引:0
|
作者
Olalekan Michael Ogundele
Adams Olalekan Omoaghe
Duyilemi Chris Ajonijebu
Abiodun Ayodele Ojo
Temitope Deborah Fabiyi
Olayemi Joseph Olajide
Deborah Tolulope Falode
Philip Adeyemi Adeniyi
机构
[1] Afe Babalola University,Department of Anatomy, College of Medicine and Health Sciences
[2] Afe Babalola University,Department of Physiology, College of Medicine and Health Sciences
[3] Afe Babalola University,Department of Chemical Sciences, College of Sciences
[4] American Hospitals and Resorts,Department of Oncology
[5] University of Ilorin,Department of Anatomy, College of Health Sciences
来源
Metabolic Brain Disease | 2014年 / 29卷
关键词
Neuron; Glia; Neurogenesis; Proliferation; Oxidative Stress; Cortex; PVZ;
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学科分类号
摘要
Glia activation and neuroinflamation are major factors implicated in the aetiology of most neurodegenerative diseases (NDDs). Several agents and toxins have been known to be capable of inducing glia activation an inflammatory response; most of which are active substances that can cause oxidative stress by inducing production of reactive oxygen species (ROS). Neurogenesis on the other hand involves metabolic and structural interaction between neurogenic and glia cells of the periventricular zone (PVZ); a region around the third ventricle. This study investigates glia activation (GFAP), cell proliferation (Ki-67) and neuronal metabolism (NSE) during neurogenesis and oxidative stress by comparing protein expression in the PVZ against that of the parietal cortex. Adult Wistar Rats were treated with normal saline and 20 mg/Kg KCN for 7 days. The tissue sections were processed for immunohistochemistry to demonstrate glia cells (anti Rat-GFAP), cell proliferation (anti Rat-Ki-67) and neuronal metabolism (anti Rat-NSE) using the antigen retrieval method. The sections from Rats treated with cyanide showed evidence of neurodegeneration both in the PVZ and cortex. The distribution of glia cells (GFAP), Neuron specific Enolase (NSE) and Ki-67 increased with cyanide treatment, although the increases were more pronounced in the neurogenic cell area (PVZ) when compared to the cortex. This suggests the close link between neuronal metabolism and glia activation both in neurogenesis and oxidative stress.
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页码:483 / 493
页数:10
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