Does neuroinflammation fan the flame in neurodegenerative diseases?

Tamy C., Frank-Cannon, Texas A&M University; Laura T., Alto, The University of Texas Southwestern Medical Center; Fiona E., McAlpine, Cancer Research UK London Research Institute; Malu, Tansey, Emory University

Persistent URL

https://open.library.emory.edu/purl/4988gthtbj-emory

Last modified

02/20/2025

Type of Material

Article

Authors

Tamy C. Frank-Cannon, Texas A&M University

Laura T. Alto, The University of Texas Southwestern Medical Center

Fiona E. McAlpine, Cancer Research UK London Research Institute

Malu Tansey, Emory University

Language

English

Date

2009

Publisher

BioMed Central

Publication Version

Final Published Version

Copyright Statement

©2009 Frank-Cannon et al; licensee BioMed Central Ltd.

License

Creative Commons Attribution 2.0 Generic

Final Published Version (URL)

http://www.molecularneurodegeneration.com/content/4/1/47

Title of Journal or Parent Work

Molecular Neurodegeneration

ISSN

1750-1326

Volume

4

Issue

47

Abstract

While peripheral immune access to the central nervous system (CNS) is restricted and tightly controlled, the CNS is capable of dynamic immune and inflammatory responses to a variety of insults. Infections, trauma, stroke, toxins and other stimuli are capable of producing an immediate and short lived activation of the innate immune system within the CNS. This acute neuroinflammatory response includes activation of the resident immune cells (microglia) resulting in a phagocytic phenotype and the release of inflammatory mediators such as cytokines and chemokines. While an acute insult may trigger oxidative and nitrosative stress, it is typically short-lived and unlikely to be detrimental to long-term neuronal survival. In contrast, chronic neuroinflammation is a long-standing and often self-perpetuating neuroinflammatory response that persists long after an initial injury or insult. Chronic neuroinflammation includes not only long-standing activation of microglia and subsequent sustained release of inflammatory mediators, but also the resulting increased oxidative and nitrosative stress. The sustained release of inflammatory mediators works to perpetuate the inflammatory cycle, activating additional microglia, promoting their proliferation, and resulting in further release of inflammatory factors. Neurodegenerative CNS disorders, including multiple sclerosis (MS), Alzheimer's disease (AD), Parkinson's disease (PD), Huntington's disease (HD), amyotrophic lateral sclerosis (ALS), tauopathies, and age-related macular degeneration (ARMD), are associated with chronic neuroinflammation and elevated levels of several cytokines. Here we review the hallmarks of acute and chronic inflammatory responses in the CNS, the reasons why microglial activation represents a convergence point for diverse stimuli that may promote or compromise neuronal survival, and the epidemiologic, pharmacologic and genetic evidence implicating neuroinflammation in the pathophysiology of several neurodegenerative diseases.

Author Notes

Correspondence: Malú G Tansey; malu.tansey@emory.edu

Research Categories

Biology, Physiology
Health Sciences, General

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Does neuroinflammation fan the flame in neurodegenerative diseases?

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