Induction of the complement component C1qB in brain of transgenic mice with neuronal overexpression of human cyclooxygenase-2

Lauren Spielman; David Winger; Lap Ho; Paul S. Aisen; Esther Shohami; Giulio Maria Pasinetti

doi:10.1007/s004010100447

Induction of the complement component C1qB in brain of transgenic mice with neuronal overexpression of human cyclooxygenase-2

Lauren Spielman, David Winger, Lap Ho, Paul S. Aisen, Esther Shohami, Giulio Maria Pasinetti

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28 Scopus citations

Abstract

We report that overexpression of human (h) cyclooxygenase-2 h(COX-2) in the brain of a transgenic mouse line leads to selective induction of endogenous complement component C1qB expression in neurons. No detectable induction of the C3 and C4 complement components in the brain was found. Chronic treatment of mice with the selective COX-2 inhibitor nimesulide reduced the hCOX-2-mediated induction of hippocampal C1qB mRNA expression. The data suggest that neuronal COX-2 expression may influence inflammatory responses in the brain, in part through modulation of complement gene expression. Because there is extensive evidence that C1q and other complement components are involved in Alzheimer's disease (AD) neurodegeneration, this study advances our understanding of the apparent benefits of COX-2 inhibition in AD.

Original language	English
Pages (from-to)	157-162
Number of pages	6
Journal	Acta Neuropathologica
Volume	103
Issue number	2
DOIs	https://doi.org/10.1007/s004010100447
State	Published - 2002

Keywords

Alzheimer's disease
Complement
Inflammation
Nimesulide

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10.1007/s004010100447

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title = "Induction of the complement component C1qB in brain of transgenic mice with neuronal overexpression of human cyclooxygenase-2",

abstract = "We report that overexpression of human (h) cyclooxygenase-2 h(COX-2) in the brain of a transgenic mouse line leads to selective induction of endogenous complement component C1qB expression in neurons. No detectable induction of the C3 and C4 complement components in the brain was found. Chronic treatment of mice with the selective COX-2 inhibitor nimesulide reduced the hCOX-2-mediated induction of hippocampal C1qB mRNA expression. The data suggest that neuronal COX-2 expression may influence inflammatory responses in the brain, in part through modulation of complement gene expression. Because there is extensive evidence that C1q and other complement components are involved in Alzheimer's disease (AD) neurodegeneration, this study advances our understanding of the apparent benefits of COX-2 inhibition in AD.",

keywords = "Alzheimer's disease, Complement, Inflammation, Nimesulide",

author = "Lauren Spielman and David Winger and Lap Ho and Aisen, {Paul S.} and Esther Shohami and Pasinetti, {Giulio Maria}",

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T1 - Induction of the complement component C1qB in brain of transgenic mice with neuronal overexpression of human cyclooxygenase-2

AU - Spielman, Lauren

AU - Winger, David

AU - Ho, Lap

AU - Aisen, Paul S.

AU - Shohami, Esther

AU - Pasinetti, Giulio Maria

PY - 2002

Y1 - 2002

N2 - We report that overexpression of human (h) cyclooxygenase-2 h(COX-2) in the brain of a transgenic mouse line leads to selective induction of endogenous complement component C1qB expression in neurons. No detectable induction of the C3 and C4 complement components in the brain was found. Chronic treatment of mice with the selective COX-2 inhibitor nimesulide reduced the hCOX-2-mediated induction of hippocampal C1qB mRNA expression. The data suggest that neuronal COX-2 expression may influence inflammatory responses in the brain, in part through modulation of complement gene expression. Because there is extensive evidence that C1q and other complement components are involved in Alzheimer's disease (AD) neurodegeneration, this study advances our understanding of the apparent benefits of COX-2 inhibition in AD.

AB - We report that overexpression of human (h) cyclooxygenase-2 h(COX-2) in the brain of a transgenic mouse line leads to selective induction of endogenous complement component C1qB expression in neurons. No detectable induction of the C3 and C4 complement components in the brain was found. Chronic treatment of mice with the selective COX-2 inhibitor nimesulide reduced the hCOX-2-mediated induction of hippocampal C1qB mRNA expression. The data suggest that neuronal COX-2 expression may influence inflammatory responses in the brain, in part through modulation of complement gene expression. Because there is extensive evidence that C1q and other complement components are involved in Alzheimer's disease (AD) neurodegeneration, this study advances our understanding of the apparent benefits of COX-2 inhibition in AD.

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Induction of the complement component C1qB in brain of transgenic mice with neuronal overexpression of human cyclooxygenase-2

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Keywords

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