The Protective Effect of INH&lt;sub&gt;2&lt;/sub&gt;BP, a Novel PARP Inhibitor 5-Iodo-6-Amino-1,2-Benzopyrone, Against Hydrogen Peroxide-Induced Apoptosis Through ERK and p38 MAPK in H9c2 Cells

Back, Oun-Cheol; Jang, Hyung-Seok; Lee, Ji-Sook; Kim, Dae Eun; Lee, Young; Park, Eun-Seok; Kim, In Sik

doi:10.1159/000439572

Cited by 10 publications

(8 citation statements)

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“…In HeLa cells, extensive activation of PARylation by MNNG specifically decreased phosphorylation of ERK1/2, which ultimately induced cell death in an ERK-dependent manner 133 . A similar effect was observed in H 2 O 2 -induced ADP-ribosylation and apoptosis in cardiomyoblasts, which correlated with a reduction in both ERK and p38 phosphorylation 160 . PARP inhibitor administration (INH 2 BP) increased phosphorylation of ERK and p38 and cell viability, led to a downregulation of ROS and pro-apoptotic factors and increased levels of anti-apoptotic proteins 160 .…”

Section: Interplay Between Mapk Signaling and Artd Family Memberssupporting

confidence: 75%

“…A similar effect was observed in H 2 O 2 -induced ADP-ribosylation and apoptosis in cardiomyoblasts, which correlated with a reduction in both ERK and p38 phosphorylation 160 . PARP inhibitor administration (INH 2 BP) increased phosphorylation of ERK and p38 and cell viability, led to a downregulation of ROS and pro-apoptotic factors and increased levels of anti-apoptotic proteins 160 . Specific ERK and p38 inhibitors individually and in combination counteracted the pro-survival effect of INH 2 BP 160 , suggesting that the pro-survival effect of this PARP inhibitor could be ascribed to both MAP kinases.…”

Section: Interplay Between Mapk Signaling and Artd Family Memberssupporting

confidence: 75%

“…PARP inhibitor administration (INH 2 BP) increased phosphorylation of ERK and p38 and cell viability, led to a downregulation of ROS and pro-apoptotic factors and increased levels of anti-apoptotic proteins 160 . Specific ERK and p38 inhibitors individually and in combination counteracted the pro-survival effect of INH 2 BP 160 , suggesting that the pro-survival effect of this PARP inhibitor could be ascribed to both MAP kinases. Of note, the ERK pathway had already been implicated in cardiac protection, while the pro-apoptotic or protective consequences of p38 signaling for the heart continue to be controversially discussed 161 .…”

Section: Interplay Between Mapk Signaling and Artd Family Membersmentioning

confidence: 99%

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Interplay between ADP-ribosyltransferases and essential cell signaling pathways controls cellular responses

2021

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Signaling cascades provide integrative and interactive frameworks that allow the cell to respond to signals from its environment and/or from within the cell itself. The dynamic regulation of mammalian cell signaling pathways is often modulated by cascades of protein post-translational modifications (PTMs). ADP-ribosylation is a PTM that is catalyzed by ADP-ribosyltransferases and manifests as mono- (MARylation) or poly- (PARylation) ADP-ribosylation depending on the addition of one or multiple ADP-ribose units to protein substrates. ADP-ribosylation has recently emerged as an important cell regulator that impacts a plethora of cellular processes, including many intracellular signaling events. Here, we provide an overview of the interplay between the intracellular diphtheria toxin-like ADP-ribosyltransferase (ARTD) family members and five selected signaling pathways (including NF-κB, JAK/STAT, Wnt-β-catenin, MAPK, PI3K/AKT), which are frequently described to control or to be controlled by ADP-ribosyltransferases and how these interactions impact the cellular responses.

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Section: Interplay Between Mapk Signaling and Artd Family Memberssupporting

confidence: 75%

Section: Interplay Between Mapk Signaling and Artd Family Memberssupporting

confidence: 75%

Section: Interplay Between Mapk Signaling and Artd Family Membersmentioning

confidence: 99%

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Interplay between ADP-ribosyltransferases and essential cell signaling pathways controls cellular responses

2021

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“…It is clearly seen that H 2 O 2 completed the autophagy and initiated the apoptotic events; however, soot alone did not induce autophagy. It is already known that H 2 O 2 induces apoptosis via cleaved caspase-3 induction ( Back et al, 2015 ; Li et al, 2015 ). In this study, soot inhibited H 2 O 2 -induced apoptosis and also inhibited cleaved caspase-3 expression and nuclear localization, suggesting its role at the transcription factor level.…”

Section: Discussionmentioning

confidence: 99%

Proliferation of Lung Epithelial Cells Is Regulated by the Mechanisms of Autophagy Upon Exposure of Soots

Niranjan

Mishra

Tripathi

et al. 2021

Front. Cell Dev. Biol.

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BackgroundSoots are known to cause many diseases in humans, but their underlying mechanisms of toxicity are still not known. Here, we report that soots induce cell proliferation of lung epithelial cells via modulating autophagy pathways.ResultsFullerene soot and diesel exhaust particles (DEP) induced cell proliferation of lung epithelial, A549 cells via distinct autophagic mechanisms and did not cause cell death. Exposure of fullerene soot protected the cell death of A549 cells, caused by hydrogen peroxide, and inhibited LPS-induced autophagy. Fullerene soot co-localized with the autophagic proteins and inhibited starvation-induced autophagy (downregulated ATG-5, beclin-1, p62, and LC3 expressions) independent of its antioxidant properties. Similarly, it decreased the expression profile of autophagic genes and upregulated the proliferation-responsive gene, Ki-67, in mice. We observed that expressions of fullerene soot-responsive genes (Beclin-1, ATG-5, and p62) were reverted by Akt Inhibitor X, indicating an important role of the Akt pathway. At an elemental level, we found that elemental carbon of fullerene soot may be converted into organic carbon, as measured by OCEC, which may point fullerene soot as a source of carbon. On the other hand, DEP upregulated the expressions of autophagy genes. Akt Inhibitor X did not attenuate DEP-induced cell proliferation and autophagic response. However, an autophagic inhibitor, chloroquine, and significantly inhibited DEP-induced cell proliferation.ConclusionIt can be said that distinct autophagic mechanisms are operational in cell proliferation of lung epithelial cells due to soots, which may be responsible for different diseases. Understanding the mechanism of these pathways provides some important targets, which can be utilized for the development of future therapeutics.

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“…It is clearly seen that, H 2 O 2 completed the autophagy and initiated the apoptotic events however soot alone did not induce autophagy. It is already known that, H 2 O 2 induces apoptosis via way of cleaved caspase-3 induction (Li et al 2015; Back et al 2015). In this study, soot has inhibited H 2 O 2 induced apoptosis and also inhibited cleaved caspase-3 expression and nuclear localization suggesting its role at transcription factor level.…”

Section: Discussionmentioning

confidence: 99%

Proliferation of lung epithelial cells is regulated by the mechanisms of autophagy upon exposure of soots

Niranjan

Mishra²,

Thakur³

2020

Preprint

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Soots are known to cause many diseases in humans but their underlying mechanisms of toxicity are still not known. Here, we report that, soots induce cell proliferation of lung epithelial cells via modulating autophagic pathways. Fullerene soot and diesel exhaust particles (DEP) induced cell proliferation of lung epithelial, A549 cells, via distinct autophagic mechanisms and did not cause cell death. Exposure of fullerene soot protected cell death of A549 cells, caused by hydrogen peroxide and inhibited LPS-induced autophagy. Fullerene soot co-localize with the autophagic proteins and inhibited starvation-induced autophagy (downregulated ATG-5, beclin-1, p62 and LC3 expressions) independent of its antioxidant properties. Similarly, it decreased expression profile of autophagic genes and upregulated proliferation responsive gene, Ki-67, in mice. We observed that, expressions of fullerene soot responsive genes (Beclin-1, ATG-5 and p62) were reverted by Akt Inhibitor X, indicating an important role of Akt pathway. On the other hand, DEP up-regulated expressions of autophagy genes. Akt Inhibitor X and Etoricoxib, did not attenuate DEP-induced cell proliferation and autophagic response. However, autophagic inhibiter 3-MA and chloroquine has significantly inhibited DEP-induced cell roliferation. In conclusion, distinct autophagic mechanisms are operational in cell proliferation of lung epithelial cells in response to soots and may have implication in diseases. The proliferation inducing potential of fullerene soot may be utilized as a regenerative agent in autophagy-associated disorders.

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The Protective Effect of INH<sub>2</sub>BP, a Novel PARP Inhibitor 5-Iodo-6-Amino-1,2-Benzopyrone, Against Hydrogen Peroxide-Induced Apoptosis Through ERK and p38 MAPK in H9c2 Cells

Cited by 10 publications

References 43 publications

Interplay between ADP-ribosyltransferases and essential cell signaling pathways controls cellular responses

Interplay between ADP-ribosyltransferases and essential cell signaling pathways controls cellular responses

Proliferation of Lung Epithelial Cells Is Regulated by the Mechanisms of Autophagy Upon Exposure of Soots

Proliferation of lung epithelial cells is regulated by the mechanisms of autophagy upon exposure of soots

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