Microglia enhance β‐amyloid peptide‐induced toxicity in cortical and mesencephalic neurons by producing reactive oxygen species

Qin, Liya; Liu, Yuxin; Cooper, Cynthia L.; Liu, Bin; Wilson, Belinda; Hong, Jau–Shyong

doi:10.1046/j.1471-4159.2002.01210.x

Cited by 280 publications

(251 citation statements)

References 45 publications

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“…Nevertheless, the dramatic protection afforded by DPI, at concentrations that do not affect other potential targets (mostly mitochondrial dehydrogenases), and by apocynin, an agent that binds at a separate site on the target enzyme, strongly suggests that this enzyme represents a major source of radical species in response to ␤A and that the selective expression of the enzyme might account in some measure for the selective effects of ␤A on astrocyte, and not neuronal, mitochondria. The importance of the NADPH oxidase in ␤A toxicity has already been suggested but with reference to the expression of the enzyme in microglia (Bianca et al, 1999;Qin et al, 2002). In the present study, however, astrocytic ROS generation seems to play a critical role in ␤A neurotoxicity, suggesting that the astrocyte may have been overlooked as a source of ROS.…”

Section: Discussionmentioning

confidence: 42%

β-Amyloid Peptides Induce Mitochondrial Dysfunction and Oxidative Stress in Astrocytes and Death of Neurons through Activation of NADPH Oxidase

Abramov

Canevari²,

Duchen³

2004

J. Neurosci.

538

372

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␤-Amyloid (␤A) peptide is strongly implicated in the neurodegeneration underlying Alzheimer's disease, but the mechanisms of neurotoxicity remain controversial. This study establishes a central role for oxidative stress by the activation of NADPH oxidase in astrocytes as the cause of ␤A-induced neuronal death. ␤A causes a loss of mitochondrial potential in astrocytes but not in neurons. The mitochondrial response consists of Ca 2ϩ -dependent transient depolarizations superimposed on a slow collapse of potential. The slow response is both prevented by antioxidants and, remarkably, reversed by provision of glutamate and other mitochondrial substrates to complexes I and II. These findings suggest that the depolarization reflects oxidative damage to metabolic pathways upstream of mitochondrial respiration. Inhibition of NADPH oxidase by diphenylene iodonium or 4-hydroxy-3-methoxy-acetophenone blocks ␤A-induced reactive oxygen species generation, prevents the mitochondrial depolarization, prevents ␤A-induced glutathione depletion in both neurons and astrocytes, and protects neurons from cell death, placing the astrocyte NADPH oxidase as a primary target of ␤A-induced neurodegeneration.

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Section: Discussionmentioning

confidence: 42%

β-Amyloid Peptides Induce Mitochondrial Dysfunction and Oxidative Stress in Astrocytes and Death of Neurons through Activation of NADPH Oxidase

Abramov

Canevari²,

Duchen³

2004

J. Neurosci.

538

372

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“…These results not only support the role of microglia in LPS-induced neurodegeneration, but they also emphasize the critical role of microglia in other models of dopaminergic neurodegeneration and Parkinson's disease. Specifically, NADPH oxidase has been implicated in the neurotoxic mechanisms of several other dopaminergic neurotoxic compounds such as rotenone (41), 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (42), and ␤-amyloid (17). Further, increased expression of NADPH oxidase has been reported in the post-mortem brains of Parkinson's disease patients (43).…”

Section: Discussionmentioning

confidence: 99%

“…First, microglia respond to toxic agents, such as the bacterial endotoxin, lipopolysaccharide (LPS), human immunodeficiency virus, type 1 coat protein gp120, and ␤-amyloid peptides, and release ROS, which in turn induce neuronal degeneration (6,(15)(16)(17). Specifically, both in vitro and in vivo studies support the possibility that microgliamediated neurotoxicity is influenced by the release of superoxide and other ROS (3,9,17,18). Alternatively, there is increasing evidence that ROS can also function as second messengers to regulate several downstream signaling molecules, including protein kinase C, mitogen-activated protein kinase, and NF-B (19 -21).…”

mentioning

confidence: 99%

NADPH Oxidase Mediates Lipopolysaccharide-induced Neurotoxicity and Proinflammatory Gene Expression in Activated Microglia

Qin

Liu

Wang

et al. 2004

Journal of Biological Chemistry

Self Cite

539

492

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Parkinson's disease is characterized by the progressive degeneration of dopaminergic neurons in the substantia nigra. We have previously reported that lipopolysaccharide (LPS)-induced degeneration of dopaminergic neurons is mediated by the release of proinflammatory factors from activated microglia. Here, we report the pivotal role of NADPH oxidase in inflammation-mediated neurotoxicity, where the LPS-induced loss of nigral dopaminergic neurons in vivo was significantly less pronounced in NADPH oxidase-deficient (PHOX

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“…75,76 As discussed earlier, this has been linked to cytokine production and neuronal death in cell cultures. [76][77][78][79][80] There are multiple b-amyloid isoforms present in the CNS, though it seems that neurotoxic properties observed in vitro are mostly attributed to the bAmyloid 1-42 isoform. 78,80 Some indicate that microglial activation is induced by aggregated b-amyloid, 81 whereas others report that diffuse forms may also be responsible for the immune response seen in this disease.…”

Section: Innate Immunity and Alzheimer's Diseasementioning

confidence: 99%

“…[76][77][78][79][80] There are multiple b-amyloid isoforms present in the CNS, though it seems that neurotoxic properties observed in vitro are mostly attributed to the bAmyloid 1-42 isoform. 78,80 Some indicate that microglial activation is induced by aggregated b-amyloid, 81 whereas others report that diffuse forms may also be responsible for the immune response seen in this disease. 82,83 Regardless, since amyloid plaques are predominantly composed of b-amyloid 1-42 , 84 this theory to explain neuronal loss in AD patients has gained much support in the field.…”

Section: Innate Immunity and Alzheimer's Diseasementioning

confidence: 99%

Neuroprotective properties of the innate immune system and bone marrow stem cells in Alzheimer's disease

2006

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The role of innate immunity and microglia in the brain is currently a matter of great debate and controversy. While several studies have provided evidence that they contribute to neurodegeneration in various animal models of brain diseases and traumas, others have shown that their inhibition may in contrast be associated with more damages or less repair. We have recently reported the existence of two different types of microglia, the resident and the newly differentiated microglia that derive from the bone marrow stem cells. Of great interest is the fact that blood-derived microglial cells are associated with amyloid plaques and these cells are able to prevent the formation or eliminate the presence of amyloid deposits in mice that develop the major hallmark of Alzheimer's disease (AD). These newly recruited cells are specifically attracted to the b-amyloid 40/42 isoforms in vivo and they participate in the elimination of these proteins by phagocytosis. This review presents the mechanisms involved in the control of the innate immune response by microglia and the beneficial properties of such a response in brain diseases, such as AD.

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Microglia enhance β‐amyloid peptide‐induced toxicity in cortical and mesencephalic neurons by producing reactive oxygen species

Cited by 280 publications

References 45 publications

β-Amyloid Peptides Induce Mitochondrial Dysfunction and Oxidative Stress in Astrocytes and Death of Neurons through Activation of NADPH Oxidase

β-Amyloid Peptides Induce Mitochondrial Dysfunction and Oxidative Stress in Astrocytes and Death of Neurons through Activation of NADPH Oxidase

NADPH Oxidase Mediates Lipopolysaccharide-induced Neurotoxicity and Proinflammatory Gene Expression in Activated Microglia

Neuroprotective properties of the innate immune system and bone marrow stem cells in Alzheimer's disease

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