Human <i>prx1</i> Gene Is a Target of Nrf2 and Is Up-regulated by Hypoxia/Reoxygenation: Implication to Tumor Biology

Kim, Yun-Jeong; Ahn, Joon-Woo; Liang, Ping; Ip, Clement; Zhang, Yuesheng; Park, Young-Mee

doi:10.1158/0008-5472.can-06-2401

Cited by 210 publications

(154 citation statements)

References 48 publications

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“…Although constitutive expression in a tumorigenic situation could be devastating because it could provide a survival advantage to invasive and metastatic cancer cells, such as the adaptation to microenvironment and the evolvement of chemoresistance in cancer cells that are known to occur in tumor hypoxia (38,39). In addition, cross-talk between tumor hypoxia and induction of Nrf2 has also been suggested recently (40). It is also noteworthy that inhibition of the Nrf2 pathway in these cancer cells enhanced sensitivity to the anti-cancer reagent cisplatin.…”

Section: Discussionmentioning

confidence: 99%

Cancer related mutations in NRF2 impair its recognition by Keap1-Cul3 E3 ligase and promote malignancy

Shibata

Ohta²,

Tong

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

647

642

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The nuclear factor E2-related factor 2 (Nrf2) is a master transcriptional activator of genes encoding numerous cytoprotective enzymes that are induced in response to environmental and endogenously derived oxidative/electrophilic agents. Under normal, nonstressed circumstances, low cellular concentrations of Nrf2 are maintained by proteasomal degradation through a Keap1-Cul3-Roc1-dependent mechanism. A model for Nrf2 activation has been proposed in which two amino-terminal motifs, DLG and ETGE, promote efficient ubiquitination and rapid turnover; known as the two-site substrate recognition/hinge and latch model. Here, we show that in human cancer, somatic mutations occur in the coding region of NRF2, especially among patients with a history of smoking or suffering from squamous cell carcinoma; in the latter case, this leads to poor prognosis. These mutations specifically alter amino acids in the DLG or ETGE motifs, resulting in aberrant cellular accumulation of Nrf2. Mutant Nrf2 cells display constitutive induction of cytoprotective enzymes and drug efflux pumps, which are insensitive to Keap1-mediated regulation. Suppression of Nrf2 protein levels by siRNA knockdown sensitized cancer cells to oxidative stress and chemotherapeutic reagents. Our results strongly support the contention that constitutive Nrf2 activation affords cancer cells with undue protection from their inherently stressed microenvironment and anti-cancer treatments. Hence, inactivation of the Nrf2 pathway may represent a therapeutic strategy to reinforce current treatments for malignancy. Congruously, the present study also provides in vivo validation of the two-site substrate recognition model for Nrf2 activation by the Keap1-Cul3-based E3 ligase.cancer cell microenvironment ͉ multidrug resistant-associated protein ͉ oxidative stress ͉ somatic mutation ͉ ubiquitin-proteasome system

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Section: Discussionmentioning

confidence: 99%

Cancer related mutations in NRF2 impair its recognition by Keap1-Cul3 E3 ligase and promote malignancy

Shibata

Ohta²,

Tong

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

647

642

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“…Phosphorylation of PrxI and II by cdc2/cyclin B complexes regulates oligomeric transitions and peroxidase activity, providing yet another mechanism to control the activity and structural state of these enzymes during the cell cycle. Changes in Prx mRNA and protein expression levels occur in many disease states, including cancer [74][75][76][77], suggesting that control of Prx function is regulated at both transcriptional and post-translational levels. While these observations show that the biological functions of individual Prxs exceed the mere reduction of H 2 O 2 , additional investigation is needed to define the array of protein complexes that include Prxs in mammalian cells, and to understand how changes in oxidation state and structural transitions of Prxs contribute to signal transduction in specific regulatory networks.…”

Section: Control Of H 2 O 2 Tonementioning

confidence: 99%

Redox-based regulation of signal transduction: Principles, pitfalls, and promises

Janssen–Heininger¹,

Mossman²,

Heintz³

et al. 2008

Free Radical Biology and Medicine

698

652

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“…The ARE was first identified as cis-element in the upstream regulatory region of the GSTA2 gene (5) and was found in the promoters of detoxifying enzyme genes such as glutathione S-transferases (6), NAD(P)H:quinone oxidoreductases (NQOs) (7,8), gastrointestinal glutathione peroxidase (9), and peroxiredoxin1 (10). The ARE is recognized by a subset of Cap'n'Collarcontaining basic leucine zipper proteins, nuclear factor erythroid 2-related factors (Nrfs), including Nrf1, Nrf2, and Nrf3.…”

mentioning

confidence: 99%

An Auto-regulatory Loop between Stress Sensors INrf2 and Nrf2 Controls Their Cellular Abundance

Lee

Jain

Papusha

et al. 2007

Journal of Biological Chemistry

177

117

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The endogenous cellular antioxidant defense system plays an important role in protecting cells from various external and internal stresses caused by xenobiotics and drugs (1), inflammation (2), and ionizing radiation (3). The perturbation of these cytoprotective regulations causes the accumulation of reactive oxygen species or electrophilic insults contributing to the pathogenesis of various diseases such as cancer, neurodegenerative disease, and atherosclerosis. Proper detoxification is mediated by the immediate expression of antioxidant proteins and phase 2 detoxifying enzymes through the activation of antioxidant-response element (ARE) 2 -binding transcription factors (4).The ARE was first identified as cis-element in the upstream regulatory region of the GSTA2 gene (5) and was found in the promoters of detoxifying enzyme genes such as glutathione S-transferases (6), NAD(P)H:quinone oxidoreductases (NQOs) (7,8), gastrointestinal glutathione peroxidase (9), and peroxiredoxin1 (10). The ARE is recognized by a subset of Cap'n'Collarcontaining basic leucine zipper proteins, nuclear factor erythroid 2-related factors (Nrfs), including Nrf1, Nrf2, and Nrf3. Among the three protein factors, Nrf2 is most potent transcription factor in regulation of basal and induced expression of antioxidant enzyme genes (11). Gene deletion studies also supported the important function of Nrf2 in cellular protection against oxidative stress and neoplasia (12).Under homeostatic conditions, Nrf2 resides predominantly within the cytoplasm of the cells by an interaction between Nrf2 and actin-bound cytosolic protein, INrf2 (inhibitor of Nrf2) or Keap1 (Kelch-like ECH-associated protein 1) (13-15). INrf2 functions as a substrate adaptor protein for a Cul3-dependent ubiquitin-protein isopeptide ligase complex to maintain the steady-state levels of Nrf2 (16). It is also believed that Nrf2 is rapidly degraded by INrf2-mediated ubiquitination because Nrf2 is barely detected in the cytoplasm. However, the exposure to oxidative stress leads to dissociation of Nrf2 from INrf2. Nrf2 is stabilized, translocates into the nucleus, and activates transcription of a battery of antioxidant genes. Recently, the mechanisms by which Nrf2 is released from INrf2 under stress have been actively investigated. One mechanism is that antioxidantinduced protein kinase C phosphorylation of serine 40 in Nrf2 leads to dissociation of Nrf2 from INrf2 (17,18). In addition, several protein kinases, including mitogen-activated protein kinase, phosphatidylinositol 3-kinase, and PKR-like endoplasmic reticulum kinase have also been involved in post-translational modification of Nrf2 and activation of Nrf2 (11,19). On the other hand, cysteine thiol groups of INrf2 were shown to function as sensors for oxidative stress that are modified by the chemical inducers, causing formation of disulfide bonds between cysteines of two INrf2 peptides. This results in conformational change that renders INrf2 unable to bind to Nrf2 (20,21). The free Nrf2 translocates to the nucleus and acti...

show abstract

Human prx1 Gene Is a Target of Nrf2 and Is Up-regulated by Hypoxia/Reoxygenation: Implication to Tumor Biology

Cited by 210 publications

References 48 publications

Cancer related mutations in NRF2 impair its recognition by Keap1-Cul3 E3 ligase and promote malignancy

Cancer related mutations in NRF2 impair its recognition by Keap1-Cul3 E3 ligase and promote malignancy

Redox-based regulation of signal transduction: Principles, pitfalls, and promises

An Auto-regulatory Loop between Stress Sensors INrf2 and Nrf2 Controls Their Cellular Abundance

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