2014
DOI: 10.1128/mcb.01408-13
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Notch-Nrf2 Axis: Regulation of Nrf2 Gene Expression and Cytoprotection by Notch Signaling

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Cited by 115 publications
(102 citation statements)
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“…These mice displayed resistance against acetaminophen, as adjudged by protection against elevated serum ALT levels. However, when the Nrf2 gene was disrupted from these mice, the protective effect against acetaminophen hepatotoxicity evoked by enhanced Notch signaling was eliminated [44]. This result indicated that the cytoprotective effect of Notch signaling might be mediated through Nrf2 signaling.…”
Section: Notch To Nrf2 Signalingmentioning
confidence: 64%
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“…These mice displayed resistance against acetaminophen, as adjudged by protection against elevated serum ALT levels. However, when the Nrf2 gene was disrupted from these mice, the protective effect against acetaminophen hepatotoxicity evoked by enhanced Notch signaling was eliminated [44]. This result indicated that the cytoprotective effect of Notch signaling might be mediated through Nrf2 signaling.…”
Section: Notch To Nrf2 Signalingmentioning
confidence: 64%
“…To this end, Nrf2 expression levels in liver specific NICD overexpressing mice (Rosa NICD/− ::AlbCre) were analyzed. It became evident that Notch to Nrf2 signaling was also functional in vivo [44]. All members of the Notch family can produce NICDs that act as transcriptional co-factors.…”
Section: Notch To Nrf2 Signalingmentioning
confidence: 99%
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“…CCN6 acts like a brake on ETC activity and ATP synthesis, whereas Nrf2, which is a facilitator of mitochondrial metabolism (Holmstrom et al, 2013;Ludtmann et al, 2014;Piantadosi et al, 2008), possibly coordinates with CCN6 by repressing its expression. The transcriptional co-activator PGC1α, which is turned on by accumulated ROS from enhanced ETC activity in a muted-CCN6 background, might be able to promote expression of Nrf2 through its influence on Notch signaling (Sawada et al, 2014;Wakabayashi et al, 2014), and Nrf2 could repress CCN6 function furthermore.…”
Section: Discussionmentioning
confidence: 99%
“…Subsequently, Keap1 translocates into the nucleus and escorts nuclear export of Nrf2 for continuous proteasomal degradation in the cytoplasm, thus terminating Nrf2 activation. 3,4 Moreover, Keap1 can interact with other proteins and Nrf2 activity can be regulated by Keap1-independent mechanisms, [5][6][7] indicating their independent regulation and roles in different biological or pathological processes.…”
Section: Introductionmentioning
confidence: 99%