Inflammatory process in Alzheimer's Disease

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Abstract

Alzheimer Disease (AD) is a neurodegenerative disorder and the most common form of dementia. Histopathologically is characterized by the presence of two major hallmarks, the intracellular neurofibrillary tangles (NFTs) and extracellular neuritic plaques (NPs) surrounded by activated astrocytes and microglia. NFTs consist of paired helical filaments of truncated tau protein that is abnormally hyperphosphorylated. The main component in the NP is the amyloid-β peptide (Aβ), a small fragment of 40–42 amino acids with a molecular weight of 4 kD. It has been proposed that the amyloid aggregates and microglia activation are able to favor the neurodegenerative process observed in AD patients. However, the role of inflammation in AD is controversial, because in early stages the inflammation could have a beneficial role in the pathology, since it has been thought that the microglia and astrocytes activated could be involved in Aβ clearance. Nevertheless the chronic activation of the microglia has been related with an increase of Aβ and possibly with tau phosphorylation. Studies in AD brains have shown an upregulation of complement molecules, pro-inflammatory cytokines, acute phase reactants and other inflammatory mediators that could contribute with the neurodegenerative process. Clinical trials and animal models with non-steroidal anti-inflammatory drugs (NSAIDs) indicate that these drugs may decrease the risk of developing AD and apparently reduce Aβ deposition. Finally, further studies are needed to determine whether treatment with anti-inflammatory strategies, may decrease the neurodegenerative process that affects these patients.

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Inflammation and Alzheimer's disease.

H Akiyama, S. Barger, S Barnum … (2000)

Inflammation clearly occurs in pathologically vulnerable regions of the Alzheimer's disease (AD) brain, and it does so with the full complexity of local peripheral inflammatory responses. In the periphery, degenerating tissue and the deposition of highly insoluble abnormal materials are classical stimulants of inflammation. Likewise, in the AD brain damaged neurons and neurites and highly insoluble amyloid beta peptide deposits and neurofibrillary tangles provide obvious stimuli for inflammation. Because these stimuli are discrete, microlocalized, and present from early preclinical to terminal stages of AD, local upregulation of complement, cytokines, acute phase reactants, and other inflammatory mediators is also discrete, microlocalized, and chronic. Cumulated over many years, direct and bystander damage from AD inflammatory mechanisms is likely to significantly exacerbate the very pathogenic processes that gave rise to it. Thus, animal models and clinical studies, although still in their infancy, strongly suggest that AD inflammation significantly contributes to AD pathogenesis. By better understanding AD inflammatory and immunoregulatory processes, it should be possible to develop anti-inflammatory approaches that may not cure AD but will likely help slow the progression or delay the onset of this devastating disorder.

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Reactive oxygen species promote TNFalpha-induced death and sustained JNK activation by inhibiting MAP kinase phosphatases.

Hideaki Kamata, Shi-Ichi Honda, Shin Maeda … (2005)

TNFalpha is a pleiotropic cytokine that induces either cell proliferation or cell death. Inhibition of NF-kappaB activation increases susceptibility to TNFalpha-induced death, concurrent with sustained JNK activation, an important contributor to the death response. Sustained JNK activation in NF-kappaB-deficient cells was suggested to depend on reactive oxygen species (ROS), but how ROS affect JNK activation was unclear. We now show that TNFalpha-induced ROS, whose accumulation is suppressed by mitochondrial superoxide dismutase, cause oxidation and inhibition of JNK-inactivating phosphatases by converting their catalytic cysteine to sulfenic acid. This results in sustained JNK activation, which is required for cytochrome c release and caspase 3 cleavage, as well as necrotic cell death. Treatment of cells or experimental animals with an antioxidant prevents H(2)O(2) accumulation, JNK phosphatase oxidation, sustained JNK activity, and both forms of cell death. Antioxidant treatment also prevents TNFalpha-mediated fulminant liver failure without affecting liver regeneration.

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Adult mouse astrocytes degrade amyloid-beta in vitro and in situ.

Tony Wyss-Coray, John Loike, Thomas Brionne … (2003)

Alzheimer disease (AD) is a progressive neurodegenerative disorder characterized by excessive deposition of amyloid-beta (Abeta) peptides in the brain. One of the earliest neuropathological changes in AD is the accumulation of astrocytes at sites of Abeta deposition, but the cause or significance of this cellular response is unclear. Here we show that cultured adult mouse astrocytes migrate in response to monocyte chemoattractant protein-1 (MCP-1), a chemokine present in AD lesions, and cease migration upon interaction with immobilized Abeta(1-42). We also show that astrocytes bind and degrade Abeta(1-42). Astrocytes plated on Abeta-laden brain sections from a mouse model of AD associate with the Abeta deposits and reduce overall Abeta levels in these sections. Our results suggest a novel mechanism for the accumulation of astrocytes around Abeta deposits, indicate a direct role for astrocytes in degradation of Abeta and implicate deficits in astroglial clearance of Abeta in the pathogenesis of AD. Treatments that increase removal of Abeta by astrocytes may therefore be a critical mechanism to reduce the neurodegeneration associated with AD.

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Author and article information

Journal

Journal ID (nlm-ta): Front Integr Neurosci

Journal ID (iso-abbrev): Front Integr Neurosci

Journal ID (publisher-id): Front. Integr. Neurosci.

Title: Frontiers in Integrative Neuroscience

Publisher: Frontiers Media S.A.

ISSN (Electronic): 1662-5145

Publication date (Electronic preprint): 09 June 2013

Publication date (Electronic): 13 August 2013

Publication date Collection: 2013

Volume: 7

Electronic Location Identifier: 59

Affiliations

[1] ¹Departamento de Biomedicina Molecular, Centro de Investigación y de Estudios Avanzados Mexico City, Mexico

[2] ²Departamento de Fisiología Biofísica y Neurociencias, Centro de Investigación y de Estudios Avanzados Mexico City, Mexico

[3] ³Posgrado en Ciencias Biológicas, Universidad Nacional Autónoma de México Mexico City, Mexico

[4] ⁴Departamento de Neuropatología Experimental, Instituto Nacional de Neurología y Neurocirugía Mexico City, Mexico

[5] ⁵Laboratorio Experimental de Enfermedades Neurodegenerativas, Instituto Nacional de Neurología y Neurocirugía Manuel Velasco Suárez Mexico City, Mexico

Author notes

Edited by: Beatriz Gomez-Gonzalez, Universidad Autonoma Metropolitana, Unidad Iztapalapa, Mexico

Reviewed by: Benjamín Florán, Centro de Investigación y de Estudios Avanzados del IPN, Mexico; Clorinda Arias, Universidad Nacional Autónoma de México, Mexico; Abbas Mirshafiey, Tehran University of Medical Sciences, Iran

*Correspondence: Victoria Campos-Peña, Laboratorio Experimental de Enfermedades Neurodegenerativas, Instituto Nacional de Neurología y Neurocirugía Manuel Velasco Suárez, Insurgentes Sur 3877, ZIP 14269, Mexico City, Mexico e-mail: neurovcp@ 123456ymail.com

†Present address: Marco A. Meraz-Ríos, Departamento de Biomedicina Molecular, Centro de Investigación y de Estudios Avanzados, Av. Instituto Politécnico Nacional 2508, ZIP 07360, Mexico City, Mexico

Article

DOI: 10.3389/fnint.2013.00059

PMC ID: 3741576

PubMed ID: 23964211

SO-VID: 220c0827-99b6-4189-9eda-973fe64eabe8

License:

This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

History

Date received : 04 May 2013

Date accepted : 25 July 2013

Page count

Figures: 2, Tables: 1, Equations: 0, References: 178, Pages: 15, Words: 13997

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Inflammatory process in Alzheimer's Disease

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Alternative approaches to Alzheimer's Disease

Most cited references 147

Inflammation and Alzheimer's disease.

Reactive oxygen species promote TNFalpha-induced death and sustained JNK activation by inhibiting MAP kinase phosphatases.

Adult mouse astrocytes degrade amyloid-beta in vitro and in situ.

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