Using Sensors and Generators of H<sub>2</sub>O<sub>2</sub>to Elucidate the Toxicity Mechanism of Piperlongumine and Phenethyl Isothiocyanate

Huang, Beijing K.; Langford, Troy F.; Sikes, Hadley D.

doi:10.1089/ars.2015.6482

Cited by 20 publications

(17 citation statements)

References 58 publications

(66 reference statements)

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“…The observation that inhibition of complex I by Rotenone did not lead to an increase in mitochondrial ROS in intact A549 cells (unlike HeLa cells) confirms earlier observations that A549 cells are less sensitive to ROS‐inducing drug treatment . In contrast, isolated mitochondria from A549 cells also showed a ROS increase due to Rotenone (but not PQS) treatment, confirming the frequent observation that the cellular ROS defense mechanism may be lost during mitochondrial isolation . As described earlier, the effect of PQS on cells is concentration dependent, very high PQS values (100 µmol/L) led to cell death as indicated by the penetration of DAPI into cells, and significantly increased cellular and nuclear ROS values.…”

Section: Discussionsupporting

confidence: 87%

“…Future experiments must show whether the PQS effect on complex III is actually due only to the effect of a class B inhibitor or is also related to the iron‐chelating effect attributed to PQS . The observation that inhibition of complex I by Rotenone did not lead to an increase in mitochondrial ROS in intact A549 cells (unlike HeLa cells) confirms earlier observations that A549 cells are less sensitive to ROS‐inducing drug treatment . In contrast, isolated mitochondria from A549 cells also showed a ROS increase due to Rotenone (but not PQS) treatment, confirming the frequent observation that the cellular ROS defense mechanism may be lost during mitochondrial isolation .…”

Section: Discussionsupporting

confidence: 82%

“…44 In contrast, isolated mitochondria from A549 cells also showed a ROS increase due to Rotenone (but not PQS) treatment, confirming the frequent observation that the cellular ROS defense mechanism may be lost during mitochondrial isolation. 44 As described earlier, 29 the effect of PQS on cells is concentration dependent, very high PQS values (100 µmol/L) led to cell death as indicated by the penetration of DAPI into cells, and significantly increased cellular and nuclear ROS values. In summary, we conclude that PQS at concentrations as in the sputum range of CF patients is sufficient to inhibit complex I at the I Q site without stimulating ROS formation.…”

Section: Discussionsupporting

confidence: 60%

“…In HeLa cells, the effect of Rotenone was different: Rotenone significantly increased superoxide levels. It has to be mentioned that the effect of Rotenone on ROS production in cells is not consistent, depending on the ROS defense, which is obviously specific in A594 cells . To investigate whether Rotenone would in principle increase ROS in A594 cells, we additionally performed inhibitor treatment with isolated mitochondria from A549 cells based on observations that the ROS defense mechanism is often lost during mitochondrial isolation .…”

Section: Resultsmentioning

confidence: 99%

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Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Rieger

Thierbach²,

Ommer-Bläsius

et al. 2020

FASEB BioAdvances

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Pseudomonas aeruginosa is a Gram‐negative bacterium of the proteobacteria class, and one of the most common causes of nosocomial infections. For example, it causes chronic pneumonia in cystic fibrosis patients. Patient sputum contains 2‐heptyl‐4‐hydroxyquinoline N‐oxide [HQNO] and Pseudomonas quorum sensing molecules such as the Pseudomonas quinolone signal [PQS]. It is known that HQNO inhibits the enzyme activity of mitochondrial and bacterial complex III at the Qi (quinone reduction) site, but the target of PQS is not known. In this work we have shown that PQS has a negative effect on mitochondrial respiration in HeLa and A549 cells. It specifically inhibits the complex I of the respiratory chain. In vitro analyses showed a partially competitive inhibition with respect to ubiquinone at the IQ site. In competing studies with Rotenone, PQS suppressed the ROS‐promoting effect of Rotenone, which is typical for a B‐type inhibitor. Prolonged incubation with PQS also had an effect on the activity of complex III.

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Section: Discussionsupporting

confidence: 87%

Section: Discussionsupporting

confidence: 82%

Section: Discussionsupporting

confidence: 60%

Section: Resultsmentioning

confidence: 99%

See 2 more Smart Citations

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Rieger

Thierbach²,

Ommer-Bläsius

et al. 2020

FASEB BioAdvances

View full text Add to dashboard Cite

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“…Efforts exist to both target existing redox-active compounds to the mitochondria and also understand the mechanisms of compounds that seem to act via the mitochondria 34,35 . Making controlled perturbations with a peroxide generator has been useful in elucidating drug mechanisms in the cytoplasm, and could be a key tool in understanding chemotherapeutics in the mitochondria 36 .…”

mentioning

confidence: 99%

Mitochondrial H₂O₂ Generation Using a Tunable Chemogenetic Tool To Perturb Redox Homeostasis in Human Cells and Induce Cell Death

2018

Self Cite

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Among reactive oxygen species (ROS), HO alone acts as a signaling molecule that promotes diverse phenotypes depending on the intracellular concentration. Mitochondria have been suggested as both sources and sinks of cellular HO, and mitochondrial dysfunction has been implicated in diseases such as cancer. A genetically encoded HO generator, d-amino acid oxidase (DAAO), was targeted to the mitochondria of human cells, and its utility in investigating cellular response to a range of HO doses over time was assessed. Organelle-specific peroxiredoxin dimerization and protein S-glutathionylation were measured as indicators of increased HO flux due to the activity of DAAO. Cell death was observed in a concentration- and time-dependent manner, and protein oxidation shifted in localization as the dose increased. This work presents the first systematic study of HO-specific perturbation of mitochondria in human cells, and it reveals a marked sensitivity of this organelle to increases in HO in comparison with prior studies that targeted the cytosol.

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TIP60 recruits SUV39H1 to chromatin to maintain heterochromatin genome stability and resist hydrogen peroxide-induced cytotoxicity

Bao

Tang

et al. 2020

GENOME INSTAB. DIS.

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Tat interacting protein 60 (TIP60) is a histone acetyltransferase involved in chromatin remodeling and the DNA damage response. However, the role of TIP60 in maintaining genome stability is poorly understood. Here, we show that TIP60 can directly interact with suppressor of variegation 3-9 homologue 1 (SUV39H1), a methyltransferase that is responsible for histone H3 tri-methylation on Lys9 (H3K9me3). When we knocked down TIP60 or treated cells with hydrogen peroxide, a typical reactive oxygen species (ROS) generator that induces genome instability, SUV39H1 dissociated from chromatin but its acetylation levels remained unchanged. Consequently, H3K9me3 levels in the heterochromatin decreased, leading to a significant increase in the expression of satellite 2 (Sat2) and α-satellite (α-Sat), indicators of heterochromatin relaxation. Micrococcal nuclease sensitivity and colony formation assays further demonstrated that TIP60 knockdown or hydrogen peroxide treatment resulted in a relaxing of the heterochromatin and genome instability. Exogenous TIP60 could rescue the assembly of SUV39H1 on chromatin and ensure genome stability in response to hydrogen peroxide. This study is the first to describe a role for TIP60 in maintaining heterochromatin structure and genome stability by recruiting SUV39H1 to the chromatin upon oxidative stress, presenting TIP60 as a promising target to sensitize cancer cells to ROS-promoting therapies.

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Using Sensors and Generators of H₂O₂to Elucidate the Toxicity Mechanism of Piperlongumine and Phenethyl Isothiocyanate

Cited by 20 publications

References 58 publications

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Mitochondrial H₂O₂ Generation Using a Tunable Chemogenetic Tool To Perturb Redox Homeostasis in Human Cells and Induce Cell Death

TIP60 recruits SUV39H1 to chromatin to maintain heterochromatin genome stability and resist hydrogen peroxide-induced cytotoxicity

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Using Sensors and Generators of H2O2to Elucidate the Toxicity Mechanism of Piperlongumine and Phenethyl Isothiocyanate

Cited by 20 publications

References 58 publications

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I Q site of mitochondrial complex I

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I Q site of mitochondrial complex I

Mitochondrial H2O2 Generation Using a Tunable Chemogenetic Tool To Perturb Redox Homeostasis in Human Cells and Induce Cell Death

TIP60 recruits SUV39H1 to chromatin to maintain heterochromatin genome stability and resist hydrogen peroxide-induced cytotoxicity

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Using Sensors and Generators of H₂O₂to Elucidate the Toxicity Mechanism of Piperlongumine and Phenethyl Isothiocyanate

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Pseudomonas Quinolone Signal molecule PQS behaves like a B Class inhibitor at the I _Q site of mitochondrial complex I

Mitochondrial H₂O₂ Generation Using a Tunable Chemogenetic Tool To Perturb Redox Homeostasis in Human Cells and Induce Cell Death