Your search keyword '"Santin, Yohan"' showing total 5 results

1. Oleuropein Aglycone Protects against MAO-A-Induced Autophagy Impairment and Cardiomyocyte Death through Activation of TFEB.

Author

Miceli C, Santin Y, Manzella N, Coppini R, Berti A, Stefani M, Parini A, Mialet-Perez J, and Nediani C

Subjects

Animals, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors antagonists & inhibitors, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Cell Nucleus metabolism, Iridoid Glucosides, Microscopy, Fluorescence, Monoamine Oxidase genetics, Myocytes, Cardiac cytology, Myocytes, Cardiac drug effects, Myocytes, Cardiac metabolism, RNA Interference, RNA, Small Interfering metabolism, Rats, Reactive Oxygen Species metabolism, Tyramine pharmacology, Autophagy drug effects, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors metabolism, Iridoids pharmacology, Monoamine Oxidase metabolism, Protective Agents pharmacology

Abstract

Age-associated diseases such as neurodegenerative and cardiovascular disorders are characterized by increased oxidative stress associated with autophagy dysfunction. Oleuropein aglycone (OA), the main polyphenol found in olive oil, was recently characterized as an autophagy inducer and a promising agent against neurodegeneration. It is presently unknown whether OA can have beneficial effects in a model of cardiac stress characterized by autophagy dysfunction. Here, we explored the effects of OA in cardiomyocytes with overexpression of monoamine oxidase-A (MAO-A). This enzyme, by degrading catecholamine and serotonin, produces hydrogen peroxide (H 2 O 2 ), which causes oxidative stress, autophagic flux blockade, and cell necrosis. We observed that OA treatment counteracted the cytotoxic effects of MAO-A through autophagy activation, as displayed by the increase of autophagic vacuoles and autophagy-specific markers (Beclin1 and LC3-II). Moreover, the decrease in autophagosomes and the increase in autolysosomes, indicative of autophagosome-lysosome fusion, suggested a restoration of the defective autophagic flux. Most interestingly, we found that the ability of OA to confer cardioprotection through autophagy induction involved nuclear translocation and activation of the transcriptional factor EB (TFEB). Our data provide strong evidence of the beneficial effects of OA, suggesting its potential use as a nutraceutical agent against age-related pathologies involving autophagy dysfunction, including cardiovascular diseases.

Published

2018

2. Roles of oxidative stress and its derivatives in the pathophysiological mechanisms of heart failure

Author

Santin, Yohan, Institut des Maladies Métaboliques et Cardiovasculaires (I2MC), Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Institut National de la Santé et de la Recherche Médicale (INSERM), Université Paul Sabatier - Toulouse III, Jeanne Mialet-Perez, and STAR, ABES

Subjects

Insuffisance cardiaque, Stress oxydant, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Oxidative stress, Autophagy, Mitochondries, Autophagie, Heart failure, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, Mitochondria, MAO-A

Abstract

Heart failure (HF) is a leading cause of death in industrialized countries. Although the intrinsic mechanisms are complex, oxidative stress has been described as a key player in the progression of ventricular dysfunction during the pathology. Thus, the team has been interested in monoamine oxidase A (MAO-A), an enzyme located at the outer mitochondrial membrane, which is the main degradation pathway for catecholamines and serotonin. In recent years, MAO-A has been identified as a major source of oxidative stress in the heart. The aim of this thesis was to better characterize the mechanisms of action of MAO-A, oxidative stress and its downstream effectors in cardiac remodeling, which would constitute an important advance in the understanding of HF pathophysiology.In the first part, we were interested in chronic myocardial infarction (MI), which is the main leading cause of HF. We observed that MAO-A was activated during chronic ischemia in patients as well as in mice, and this activation was involved in post-MI deleterious remodeling. From a mechanistic point of view, we saw that MAO-A activation promoted mitochondrial accumulation of 4-hydroxynonenal (4-HNE), a highly reactive aldehyde, through intra-mitochondrial lipid peroxidation. This accumulation triggered 4-HNE binding on specific mitochondrial targets, favoring calcium overload within the organelle, alteration of the respiratory chain and energetic failure, further contributing to deleterious post-MI remodeling. This study therefore highlighted the key role of mitochondrial dysfunction in MAO-A-induced damage. In a second part, we sought to characterize the consequences of long-term MAO-A overactivation on mitochondrial quality control. Indeed, dysfunctional mitochondria are normally eliminated by the autophagy-lysosome pathway, but studies have shown that this pathway is progressively impaired during HF. Our results showed that MAO-A activation led to an alteration of lysosomal acidification and a lack of nuclear translocation of the transcription factor EB (TFEB), a “master regulator” of autophagy and lysosomal biogenesis. As a result, we observed a blockade of autophagic flux leading to cardiomyocyte necrosis. Interestingly, TFEB overexpression in MAO-A-overexpressing mice mitigated autophagosomes accumulation, mitochondrial fission, cardiomyocytes death and cardiac dysfunction, which spontaneously occur in this mouse model. Despite these very exciting results, this project highlighted a dramatic lack of lysosomotropic tools that could be used in research and/or as therapeutic tools. We thus collaborated with the company « Chromalys » in order to develop nanoparticles (NPs) able to (re)acidify lysosomes with an altered pH. After showing a lysosomal addressing of these NPs, we evaluated their functional consequences on cells treated with doxorubicin, a clinically used anthracycline which has been pointed to alter lysosomal pH in cardiac cells. We observed that NPs improved lysosomal acidification, autophagic flux and cell viability that were altered by doxorubicin, making these NPs very interesting tools in the study of lysosomal alteration and in the restoration of their function. This thesis dealt with several axes corresponding to different HF aspects and brought new advances on the understanding of the pathophysiological mechanisms of this complex disease. It has also allowed the identification of potentially interesting therapeutic tools that could open new tracks in HF treatment., L’insuffisance cardiaque (IC) est une cause majeure de mortalité dans les pays industrialisés. Bien que les mécanismes intrinsèques de l’IC soient complexes, il a été démontré que le stress oxydant était un déterminant essentiel dans la progression de la dysfonction ventriculaire au cours de la pathologie. En ce sens, l’équipe s’est intéressée à la monoamine oxydase A (MAO-A), une enzyme située au niveau de la membrane externe mitochondriale, qui constitue la principale voie de dégradation des catécholamines et de la sérotonine. Au cours des dernières années, la MAO-A a été identifiée comme une source importante de stress oxydant dans le cœur. Le but de cette thèse a été de mieux caractériser les mécanismes d’action de la MAO-A, du stress oxydant et de ses effecteurs dans l’altération cardiaque, ce qui pourrait constituer une avancée importante dans la compréhension des mécanismes physiopathologiques de l’IC. Dans une première partie, nous nous sommes intéressés à l’infarctus du myocarde (IDM) chronique qui constitue la cause principale d’IC. Nous avons observé que la MAO-A était activée au cours de l’ischémie chronique chez des patients ainsi que chez des souris, et que cette activation participait au remodelage délétère post-IDM. D’un point de vue mécanistique, nous avons montré que l’activation de la MAO-A favorisait l’accumulation mitochondriale de 4-hydroxynonénal (4-HNE), un aldéhyde très réactif, via une peroxydation lipidique intra-mitochondriale. Cette accumulation a conduit à la fixation du 4-HNE sur certaines cibles mitochondriales, favorisant une surcharge calcique dans l’organite, une altération de la chaîne respiratoire et un déficit énergétique, qui participent au remodelage délétère post-IDM. Cette étude a donc permis de mettre en évidence le rôle clé de la dysfonction mitochondriale dans les dommages induits par la MAO-A. Dans une deuxième partie, nous avons cherché à caractériser les conséquences de la suractivation de la MAO-A sur le contrôle qualité mitochondrial à long terme. Les mitochondries dysfonctionnelles sont normalement éliminées par la voie autophagie-lysosome, mais des études ont montré que cette voie était progressivement altérée dans l’IC. Nos travaux ont montré que l’activation chronique de la MAO-A entrainait une altération de l’acidification lysosomale et un défaut de translocation nucléaire du facteur de transcription EB (TFEB), un « master régulateur » de l'autophagie et de la biogenèse des lysosomes.

Published

2019

3. Rôles du stress oxydant et de ses dérivés dans les mécanismes physiopathologiques de l’insuffisance cardiaque

Author

Santin, Yohan, Institut des Maladies Métaboliques et Cardiovasculaires (I2MC), Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Institut National de la Santé et de la Recherche Médicale (INSERM), Université Paul Sabatier - Toulouse III, and Jeanne Mialet-Perez

Subjects

Insuffisance cardiaque, Stress oxydant, Oxidative stress, Autophagy, Mitochondries, Autophagie, Heart failure, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, Mitochondria, MAO-A

Abstract

Heart failure (HF) is a leading cause of death in industrialized countries. Although the intrinsic mechanisms are complex, oxidative stress has been described as a key player in the progression of ventricular dysfunction during the pathology. Thus, the team has been interested in monoamine oxidase A (MAO-A), an enzyme located at the outer mitochondrial membrane, which is the main degradation pathway for catecholamines and serotonin. In recent years, MAO-A has been identified as a major source of oxidative stress in the heart. The aim of this thesis was to better characterize the mechanisms of action of MAO-A, oxidative stress and its downstream effectors in cardiac remodeling, which would constitute an important advance in the understanding of HF pathophysiology.In the first part, we were interested in chronic myocardial infarction (MI), which is the main leading cause of HF. We observed that MAO-A was activated during chronic ischemia in patients as well as in mice, and this activation was involved in post-MI deleterious remodeling. From a mechanistic point of view, we saw that MAO-A activation promoted mitochondrial accumulation of 4-hydroxynonenal (4-HNE), a highly reactive aldehyde, through intra-mitochondrial lipid peroxidation. This accumulation triggered 4-HNE binding on specific mitochondrial targets, favoring calcium overload within the organelle, alteration of the respiratory chain and energetic failure, further contributing to deleterious post-MI remodeling. This study therefore highlighted the key role of mitochondrial dysfunction in MAO-A-induced damage. In a second part, we sought to characterize the consequences of long-term MAO-A overactivation on mitochondrial quality control. Indeed, dysfunctional mitochondria are normally eliminated by the autophagy-lysosome pathway, but studies have shown that this pathway is progressively impaired during HF. Our results showed that MAO-A activation led to an alteration of lysosomal acidification and a lack of nuclear translocation of the transcription factor EB (TFEB), a “master regulator” of autophagy and lysosomal biogenesis. As a result, we observed a blockade of autophagic flux leading to cardiomyocyte necrosis. Interestingly, TFEB overexpression in MAO-A-overexpressing mice mitigated autophagosomes accumulation, mitochondrial fission, cardiomyocytes death and cardiac dysfunction, which spontaneously occur in this mouse model. Despite these very exciting results, this project highlighted a dramatic lack of lysosomotropic tools that could be used in research and/or as therapeutic tools. We thus collaborated with the company « Chromalys » in order to develop nanoparticles (NPs) able to (re)acidify lysosomes with an altered pH. After showing a lysosomal addressing of these NPs, we evaluated their functional consequences on cells treated with doxorubicin, a clinically used anthracycline which has been pointed to alter lysosomal pH in cardiac cells. We observed that NPs improved lysosomal acidification, autophagic flux and cell viability that were altered by doxorubicin, making these NPs very interesting tools in the study of lysosomal alteration and in the restoration of their function. This thesis dealt with several axes corresponding to different HF aspects and brought new advances on the understanding of the pathophysiological mechanisms of this complex disease. It has also allowed the identification of potentially interesting therapeutic tools that could open new tracks in HF treatment.; L’insuffisance cardiaque (IC) est une cause majeure de mortalité dans les pays industrialisés. Bien que les mécanismes intrinsèques de l’IC soient complexes, il a été démontré que le stress oxydant était un déterminant essentiel dans la progression de la dysfonction ventriculaire au cours de la pathologie. En ce sens, l’équipe s’est intéressée à la monoamine oxydase A (MAO-A), une enzyme située au niveau de la membrane externe mitochondriale, qui constitue la principale voie de dégradation des catécholamines et de la sérotonine. Au cours des dernières années, la MAO-A a été identifiée comme une source importante de stress oxydant dans le cœur. Le but de cette thèse a été de mieux caractériser les mécanismes d’action de la MAO-A, du stress oxydant et de ses effecteurs dans l’altération cardiaque, ce qui pourrait constituer une avancée importante dans la compréhension des mécanismes physiopathologiques de l’IC. Dans une première partie, nous nous sommes intéressés à l’infarctus du myocarde (IDM) chronique qui constitue la cause principale d’IC. Nous avons observé que la MAO-A était activée au cours de l’ischémie chronique chez des patients ainsi que chez des souris, et que cette activation participait au remodelage délétère post-IDM. D’un point de vue mécanistique, nous avons montré que l’activation de la MAO-A favorisait l’accumulation mitochondriale de 4-hydroxynonénal (4-HNE), un aldéhyde très réactif, via une peroxydation lipidique intra-mitochondriale. Cette accumulation a conduit à la fixation du 4-HNE sur certaines cibles mitochondriales, favorisant une surcharge calcique dans l’organite, une altération de la chaîne respiratoire et un déficit énergétique, qui participent au remodelage délétère post-IDM. Cette étude a donc permis de mettre en évidence le rôle clé de la dysfonction mitochondriale dans les dommages induits par la MAO-A. Dans une deuxième partie, nous avons cherché à caractériser les conséquences de la suractivation de la MAO-A sur le contrôle qualité mitochondrial à long terme. Les mitochondries dysfonctionnelles sont normalement éliminées par la voie autophagie-lysosome, mais des études ont montré que cette voie était progressivement altérée dans l’IC. Nos travaux ont montré que l’activation chronique de la MAO-A entrainait une altération de l’acidification lysosomale et un défaut de translocation nucléaire du facteur de transcription EB (TFEB), un « master régulateur » de l'autophagie et de la biogenèse des lysosomes.

Published

2019

4. Oxidative Stress by Monoamine Oxidase-A Impairs Transcription Factor EB Activation and Autophagosome Clearance, Leading to Cardiomyocyte Necrosis and Heart Failure.

Author

Santin, Yohan, Sicard, Pierre, Vigneron, François, Guilbeau-Frugier, Céline, Dutaur, Marianne, Lairez, Olivier, Couderc, Bettina, Manni, Diego, Korolchuk, Viktor I., Lezoualc'h, Frank, Parini, Angelo, and Mialet-Perez, Jeanne

Subjects

*HEART failure, *AUTOPHAGY, *OXIDATIVE stress, *REACTIVE oxygen species, *SEROTONIN, *NORADRENALINE

Abstract

Aims: In heart failure (HF), mitochondrial quality control and autophagy are progressively impaired, but the role of oxidative stress in this process and its underlying mechanism remain to be defined. By degrading norepinephrine and serotonin, the mitochondrial enzyme, monoamine oxidase-A (MAO-A), is a potent source of reactive oxygen species (ROS) in the heart and its activation leads to the persistence of mitochondrial damage. In this study, we analyzed the consequences of ROS generation by MAO-A on the autophagy--lysosome pathway in the heart. Results: Cardiomyocyte-driven expression of MAO-A in mice led to mitochondrial fission and translocation of Drp1 and Parkin in the mitochondrial compartment. Ventricles from MAO-A transgenic mice displayed accumulation of LC3-positive autophagosomes, together with p62 and ubiquitylated proteins, indicating impairment of autophagy. In vitro adenoviral delivery of MAO-A in cardiomyocytes and the consequent generation of ROS blocked autophagic flux with accumulation of LC3II, p62, and ubiquitylated proteins, leading to mitochondrial fission and cell necrosis. In addition, MAO-A activation induced accumulation of lysosomal proteins, cathepsin D and Lamp1, reduced lysosomal acidification, and blocked the nuclear translocation of transcription factor-EB (TFEB), a master regulator of autophagy and lysosome biogenesis. Most interestingly, overexpression of TFEB attenuated autophagosome buildup, mitochondrial fission, cardiomyocyte death, and HF associated with MAO-A activation. Innovation and Conclusion: This study unravels a new link between MAO-dependent H2O2 production and lysosomal dysfunction. Altogether, our findings demonstrate that the MAO-A/H2O2 axis has a negative impact on the elimination and recycling of mitochondria through the autophagy--lysosome pathway, which participates in cardiomyocyte death and HF. [ABSTRACT FROM AUTHOR]

Published

2016

5. Monoamine oxidases in age-associated diseases: New perspectives for old enzymes.

Author

Santin, Yohan, Resta, Jessica, Parini, Angelo, and Mialet-Perez, Jeanne

Subjects

*OXIDASES, *CELLULAR aging, *MONOAMINE transporters, *ENZYMES, *CANCER treatment, *MONOAMINE oxidase, *CENTRAL nervous system, *BIOGENIC amines

Abstract

• Monoamine oxidases overactivation is a common hallmark of several age-associated diseases. • Monoamine oxidases are involved in neurodegenerative diseases, cardiac aging, metabolic disorders and cancer, for which selective inhibitors are currently used or in development. • Increased monoamine oxidase activity leads to altered substrate (norepinephrine, dopamine, serotonin) concentrations and generates oxidative stress and aldehydes during aging. • Monoamine oxidase-dependent byproducts cause protein aggregation, cell death, mitochondrial oxidative damage and impair the different steps of mitochondrial quality control such as mitochondrial biogenesis, dynamics and autophagy in the central nervous system and the heart. Population aging is one of the most significant social changes of the twenty-first century. This increase in longevity is associated with a higher prevalence of chronic diseases, further rising healthcare costs. At the molecular level, cellular senescence has been identified as a major process in age-associated diseases, as accumulation of senescent cells with aging leads to progressive organ dysfunction. Of particular importance, mitochondrial oxidative stress and consequent organelle alterations have been pointed out as key players in the aging process, by both inducing and maintaining cellular senescence. Monoamine oxidases (MAOs), a class of enzymes that catalyze the degradation of catecholamines and biogenic amines, have been increasingly recognized as major producers of mitochondrial ROS. Although well-known in the brain, evidence showing that MAOs are also expressed in a variety of peripheral organs stimulated a growing interest in the extra-cerebral roles of these enzymes. Besides, the fact that MAO-A and/or MAO-B are frequently upregulated in aged or dysfunctional organs has uncovered new perspectives on their roles in pathological aging. In this review, we will give an overview of the major results on the regulation and function of MAOs in aging and age-related diseases, paying a special attention to the mechanisms linked to the increased degradation of MAO substrates or related to MAO-dependent ROS formation. [ABSTRACT FROM AUTHOR]

Published

2021