p53-PGC-1α Pathway Mediates Oxidative Mitochondrial Damage and Cardiomyocyte Necrosis Induced by Monoamine Oxidase-A Upregulation: Role in Chronic Left Ventricular Dysfunction in Mice

Villeneuve, Christelle; Guilbeau‐Frugier, Céline; Sicard, Pierre; Lairez, Olivier; Ordener, Catherine; Duparc, Thibaut; Paulis, Damien De; Couderc, Bettina; Spreux‐Varoquaux, Odile; Tortosa, Florence; Garnier, Anne; Knauf, Claude; Valet, Philippe; Borchi, Elisabetta; Nediani, Chiara; Gharib, Abdallah; Ovize, Michel; Delisle, Marie–Bernadette; Parini, Angelo; Mialet‐Perez, Jeanne

doi:10.1089/ars.2011.4373

Cited by 118 publications

(121 citation statements)

References 44 publications

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“…Tyr treatment induced a dose‐dependent increase in ROS production in cardiomyocytes (Figure 2e). On one hand, we found that above the concentration of 250 µM of Tyr, primary cardiomyocytes underwent cell death, consistent with our previous findings (Villeneuve et al, 2013) (Figure 2f). On the other hand, at doses of 100, 50 and 10 µM, no cytotoxicity was observed with Tyr up to 72 hr (Figure 2f).…”

Section: Resultssupporting

confidence: 93%

“…These particular responses might depend on the cell type and on the amount of H 2 O 2 , which is known to drive dose‐dependent cellular effects (Duan, Duan, Zhang, & Tong, 2005; Giorgio et al, 2007). During cardiac ischaemia‐reperfusion injury, where high levels of MAO substrates are released, and in the hearts of transgenic mice overexpressing MAO‐A, cell apoptosis and necrosis are preferentially activated together with the lysosomal alteration‐induced blockade of the autophagic flux (Bianchi et al, 2005; Santin et al, 2016; Villeneuve et al, 2013). Here, we demonstrate that chronic sublethal doses of H 2 O 2 produced by MAO‐A in response to its endogenous (NE) or exogenous (Tyr) substrates can recapitulate all the features of senescence.…”

Section: Discussionmentioning

confidence: 99%

“…Here, we demonstrate that chronic sublethal doses of H 2 O 2 produced by MAO‐A in response to its endogenous (NE) or exogenous (Tyr) substrates can recapitulate all the features of senescence. This could have particular relevance in cardiac ageing, where MAO‐A is likely to be chronically activated due to: (a) sympathetic activation and enhanced release of norepinephrine from adrenergic nerves (Santulli & Iaccarino, 2016); and (b) overexpression of MAO‐A in the ageing heart (as shown in Figure 1a,b) or in age‐associated cardiac diseases (Manni et al, 2016; Villeneuve et al, 2013). In addition, the role of MAO‐A in senescence could be extended to different cell types, since MAO‐A has been characterized in many proliferative cells, such as fibroblasts and bone marrow mesenchymal stem cells, where its expression was significantly increased during ageing (Edelstein & Breakefield, 1986; Trouche et al, 2010).…”

Section: Discussionmentioning

confidence: 99%

“…In the heart, MAO‐A has been demonstrated to be an important source of oxidative stress in acute and chronic pathological conditions (Bianchi et al, 2005; Kaludercic et al, 2010). In particular, cardiac overexpression of MAO‐A drives oxidative stress and mitochondrial damage, leading to cell death and heart failure (Kaludercic, Mialet‐Perez, Paolocci, Parini, & Di Lisa, 2014; Villeneuve et al, 2013). Notably, all these effects are observed with high levels of MAO‐A activation, and it is well‐established that depending on its concentration, H 2 O 2 can have multiple dose‐dependent cellular responses, ranging from proliferation to necrosis (Giorgio, Trinei, Migliaccio, & Pelicci, 2007).…”

Section: Introductionmentioning

confidence: 99%

“…Notably, all these effects are observed with high levels of MAO‐A activation, and it is well‐established that depending on its concentration, H 2 O 2 can have multiple dose‐dependent cellular responses, ranging from proliferation to necrosis (Giorgio, Trinei, Migliaccio, & Pelicci, 2007). p53 is one of the main effectors of the MAO‐A/H 2 O 2 axis (Villeneuve et al, 2013), which is at the crossroad of numerous signalling pathways and, depending on the extent of damage, can initiate DNA repair, senescence or cell death (Green & Kroemer, 2009). These observations, together with the fact that MAO‐A expression increases in the ageing heart (Maurel et al, 2003), led us to investigate whether a chronic increase in H 2 O 2 through persistent MAO‐A activation could drive senescence in cardiac cells.…”

Section: Introductionmentioning

confidence: 99%

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Monoamine oxidase‐A is a novel driver of stress‐induced premature senescence through inhibition of parkin‐mediated mitophagy

et al. 2018

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Cellular senescence, the irreversible cell cycle arrest observed in somatic cells, is an important driver of age‐associated diseases. Mitochondria have been implicated in the process of senescence, primarily because they are both sources and targets of reactive oxygen species (ROS). In the heart, oxidative stress contributes to pathological cardiac ageing, but the mechanisms underlying ROS production are still not completely understood. The mitochondrial enzyme monoamine oxidase‐A (MAO‐A) is a relevant source of ROS in the heart through the formation of H2O2 derived from the degradation of its main substrates, norepinephrine (NE) and serotonin. However, the potential link between MAO‐A and senescence has not been previously investigated. Using cardiomyoblasts and primary cardiomyocytes, we demonstrate that chronic MAO‐A activation mediated by synthetic (tyramine) and physiological (NE) substrates induces ROS‐dependent DNA damage response, activation of cyclin‐dependent kinase inhibitors p21cip, p16ink4a, and p15ink4b and typical features of senescence such as cell flattening and SA‐β‐gal activity. Moreover, we observe that ROS produced by MAO‐A lead to the accumulation of p53 in the cytosol where it inhibits parkin, an important regulator of mitophagy, resulting in mitochondrial dysfunction. Additionally, we show that the mTOR kinase contributes to mitophagy dysfunction by enhancing p53 cytoplasmic accumulation. Importantly, restoration of mitophagy, either by overexpression of parkin or inhibition of mTOR, prevents mitochondrial dysfunction and induction of senescence. Altogether, our data demonstrate a novel link between MAO‐A and senescence in cardiomyocytes and provides mechanistic insights into the potential role of MAO‐dependent oxidative stress in age‐related pathologies.

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Section: Resultssupporting

confidence: 93%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Monoamine oxidase‐A is a novel driver of stress‐induced premature senescence through inhibition of parkin‐mediated mitophagy

et al. 2018

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Platelet activation and arterial peripheral serotonin turnover in cardiac remodeling associated to aortic stenosis

et al. 2014

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Peripheral serotonin (5-HT) has been involved in adverse cardiac remodeling and valve fibrosis. The peripheral levels of 5-HT mainly depend on its release from activated platelets and degradation by monoamine oxidase A (MAO-A). The SERAOPI study investigated the relationship between arterial serotoninergic system, degree of platelet activation and cardiac remodeling, in patients with aortic valve stenosis (AS). Thirty patients with severe AS and 15 control subjects underwent transthoracic echocardiography, radial, and aortic arterial blood sampling. Measurements of 5-HT and its MAO-Adependent degradation product, 5-HIAA, were performed by HPLC. Arterial platelet activation was assessed by flow cytometry analysis of platelet surface expression of P-selectin and activated integrin GPIIb/IIIa. Activated platelets and arterial plasma 5-HT increased in AS patients as compared to control subjects (P-selectin 1.08 6 0.2MFI vs. 0.49 6 0.1MFI, P 5 0.04; GPIIb/IIIa 0.71 6 0.1MFI vs. 0.35 6 0.1MFI; P 5 0.0015 and arterial plasma 5-HT 11.55 6 1.6 nM vs. 6.18 6 0.7 nM, P 5 0.028, respectively). Moreover, 5-HT was strongly correlated to left ventricular hypertrophy assessed by echocardiography. The correlation was independent of cardiovascular risk comorbidities and others echocardiographic AS parameters. Finally, plasma 5-HIAA increased in AS patients (74.64 6 9.7 nM vs. 37.16 6 4.1 nM; P 5 0.0002) indicating a higher 5-HT degradation rate by MAO-A. Platelet activation, arterial circulating serotonin, and serotonin degradation increased in patients with AS. These observations suggest that the serotoninergic system may contribute to the pathogenesis of AS including valve fibrosis and adverse ventricular remodeling.

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Cardiac troponins—Translational biomarkers in cardiology: Theory and practice of cardiac troponin high‐sensitivity assays

et al. 2016

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Tn is a unique translational biomarker in cardiology whose potential has not been diminished in the new era of high sensitive assays. cTns can be valuable markers in cardiac diseases as well as in infectious diseases and respiratory diseases. Furthermore, the role of cTns is growing in the routine evaluation of cardioxicity and in determining the efficacy/safety ratio of novel cardioprotective strategies in clinical settings. cTns can detect myocardial injury not only in a wide spectrum of laboratory animals in experimental studies in vivo, but also in isolated heart models or cardiomyocytes in vitro. The crucial issue regarding the cross‐species usage of cardiac troponin investigation remains the choice of cardiac troponin testing. This review summarizes the recent proteomic data on aminoacid sequences of cTnT and cTnI in various species, as well as selected analytical characteristics of human cardiac troponin high‐sensitivity assays. Due to the highly phylogenetically conserved structure of troponins, the same bioindicator can be investigated using the same method in both clinical and experimental cardiology, thus contributing to a better understanding of the pathogenesis of cardiac diseases as well as to increased effectiveness of troponin use in clinical practice. Measuring cardiac troponins using commercially available human high‐sensitivity cardiac troponin tests with convenient antibodies selected on the basis of adequate proteomic knowledge can solve many issues which would otherwise be difficult to address in clinical settings for various ethical and practical reasons. Our survey could help elaborate the practical guidelines for optimizing the choice of cTns assay in cardiology. © 2016 BioFactors, 42(2):133–148, 2016

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p53-PGC-1α Pathway Mediates Oxidative Mitochondrial Damage and Cardiomyocyte Necrosis Induced by Monoamine Oxidase-A Upregulation: Role in Chronic Left Ventricular Dysfunction in Mice

Cited by 118 publications

References 44 publications

Monoamine oxidase‐A is a novel driver of stress‐induced premature senescence through inhibition of parkin‐mediated mitophagy

Monoamine oxidase‐A is a novel driver of stress‐induced premature senescence through inhibition of parkin‐mediated mitophagy

Platelet activation and arterial peripheral serotonin turnover in cardiac remodeling associated to aortic stenosis

Cardiac troponins—Translational biomarkers in cardiology: Theory and practice of cardiac troponin high‐sensitivity assays

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