Thrombin-Induced Oxidative Stress Contributes to the Death of Hippocampal Neurons In Vivo: Role of Microglial NADPH Oxidase

doi:10.1523/JNEUROSCI.4306-04.2005

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The Journal of Neuroscience, April 20, 2005, 25(16):4082-4090; doi:10.1523/JNEUROSCI.4306-04.2005

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Neurobiology of Disease
Thrombin-Induced Oxidative Stress Contributes to the Death of Hippocampal Neurons In Vivo: Role of Microglial NADPH Oxidase
Sang-Ho Choi, Da Yong Lee, Seung Up Kim, and Byung Kwan Jin
Neuroscience Graduate Program, Brain Disease Research Center, Ajou University School of Medicine, Suwon 443-721, Korea

The present study investigated whether thrombin, a potent microglialactivator, can induce reactive oxygen species (ROS) generationthrough activation of microglial NADPH oxidase and if this maycontribute to oxidative damage and consequent neurodegeneration.Seven days after intrahippocampal injection of thrombin, Nisslstaining and immunohistochemistry using the neuronal-specificnuclear protein NeuN revealed a significant loss in hippocampalCA1 neurons. In parallel, thrombin-activated microglia, assessedby OX-42 and OX-6 immunohistochemistry, and ROS production,assessed by hydroethidine histochemistry, were observed in thehippocampal CA1 area in which degeneration of hippocampal neuronsoccurred. Reverse transcription-PCR at various time points afterthrombin administration demonstrated an early and transientexpression of inducible nitric oxide synthase (iNOS) and severalproinflammatory cytokines. Western blot analysis and double-labelimmunohistochemistry showed an increase in the expression ofand the localization of iNOS within microglia. Additional studiesdemonstrated that thrombin induced the upregulation of membrane(gp91^phox) and cytosolic (p47^phox and p67^phox) components, translocationof cytosolic proteins (p47^phox, p67^phox, and Rac1) to the membrane,and p67^phox expression of the NADPH oxidase in microglia inthe hippocampus in vivo, indicating the activation of NADPHoxidase. The thrombin-induced oxidation of proteins and lossof hippocampal CA1 neurons were partially inhibited by an NADPHoxidase inhibitor and by an antioxidant. To our knowledge, thepresent study is the first to demonstrate that thrombin-inducedneurotoxicity in the hippocampus in vivo is caused by microglialNADPH oxidase-mediated oxidative stress. This suggests thatthrombin inhibition or enhancing antioxidants may be beneficialfor the treatment of neurodegenerative diseases, such as Alzheimer'sdisease, that are associated with microglial-derived oxidativedamage.

Key words: thrombin; hippocampus; microglia; NADPH oxidase; oxidative stress; Alzheimer's disease

Received Oct 16, 2004; revised March 8, 2005; accepted March 8, 2005.

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