2002
DOI: 10.1006/nbdi.2002.0515
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Oxidative Stress Increases Expression and Activity of BACE in NT2 Neurons

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Cited by 352 publications
(297 citation statements)
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References 36 publications
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“…This finding supports a functional role for oxidative stress in regulating the amyloidogenic response to brain trauma in vivo, and it is consistent with some in vitro data showing that oxidative stress can positively modulate APP metabolism and increase in Ab formation (Misonou et al 2000). Thus, previous studies have shown that oxidants can indeed increased BACE activity and amyloid formation in neuronal cell lines (Tamagno et al 2002).…”
Section: Discussionsupporting
confidence: 90%
“…This finding supports a functional role for oxidative stress in regulating the amyloidogenic response to brain trauma in vivo, and it is consistent with some in vitro data showing that oxidative stress can positively modulate APP metabolism and increase in Ab formation (Misonou et al 2000). Thus, previous studies have shown that oxidants can indeed increased BACE activity and amyloid formation in neuronal cell lines (Tamagno et al 2002).…”
Section: Discussionsupporting
confidence: 90%
“…These studies consistently demonstrated a strong correlation between oxidative stress and accumulation of Aβ with the possible involvement of an APP-processing enzyme, β-secretase [53][54][55][56][57]. A recent report using heterozygous Mn-SOD knockout mice also showed that oxidative stress modulates hyperphosphorylation of tau, which leads to the formation of neurofibrillary tangles [58].…”
Section: Contribution Of Complex IV Defects To Oxidative Stress and Nmentioning
confidence: 84%
“…Because the inflammatory response to A␤ peptide partly involves the CD14 immune response (Fassbender et al, 2004;Milatovic et al, 2004), and A␤ peptide can induce microglial production of superoxide (Bianca et al, 1999), one hypothesis that emerges is that EP2-mediated oxidative stress indirectly promotes increased A␤ peptide levels via increased BACE1 processing. Recent investigations have linked increases in oxidative stress to increases in BACE1 activity and production of ␤-CTF (Tamagno et al, 2002;Apelt et al, 2004). Increases in BACE1 processing have also been demonstrated in aging and AD, in which inflammation and oxidative stress are prominent features (Fukumoto et al, 2002(Fukumoto et al, , 2004Yang et al, 2003;Apelt et al, 2004;Holsinger et al, 2004).…”
Section: Discussionmentioning
confidence: 99%
“…Association of oxidative inflammatory response and increased A␤ peptide levels in APPSwe-PS1⌬E9 in EP2؉/؉ background Recent studies have demonstrated that BACE1 processing of APP is increased in aging and AD (Fukumoto et al, 2002(Fukumoto et al, , 2004Holsinger et al, 2002;Yang et al, 2003;Li et al, 2004), and this may relate to effects of increased oxidative stress on BACE1 activity (Tamagno et al, 2002;Apelt et al, 2004). EP2 receptor signaling leads to a marked inflammatory oxidative response in the LPS model of innate immunity (T. J.…”
Section: Deletion Of the Ep2 Receptor In Appswe-ps1⌬e9 Mice Reduces Lmentioning
confidence: 99%