Your search keyword '"Eduardo Makiyama Klosowski"' showing total 8 results

1. Toluidine blue O directly and photodynamically impairs the bioenergetics of liver mitochondria: a potential mechanism of hepatotoxicity

Author

Karina Borba Paulino, Dos Santos, Ana Flavia Gatto, Raimundo, Eduardo Makiyama, Klosowski, Byanca Thais Lima, de Souza, Márcio Shigueaki, Mito, Renato Polimeni, Constantin, Gislaine Cristiane, Mantovanelli, Juliana Morais, Mewes, Paulo Francisco Veiga, Bizerra, Paulo Vinicius Moreira, da Costa Menezes, Karina Sayuri, Utsunomiya, Eduardo Hideo, Gilglioni, Rogério, Marchiosi, Wanderley Dantas, Dos Santos, Osvaldo, Ferrarese-Filho, Wilker, Caetano, Paulo Cesar, de Souza Pereira, Renato Sonchini, Gonçalves, Jorgete, Constantin, Emy Luiza, Ishii-Iwamoto, and Rodrigo Polimeni, Constantin

Subjects

Physical and Theoretical Chemistry

Abstract

Toluidine blue O (TBO) is a phenothiazine dye that, due to its photochemical characteristics and high affinity for biomembranes, has been revealed as a new photosensitizer (PS) option for antimicrobial photodynamic therapy (PDT). This points to a possible association with membranous organelles like mitochondrion. Therefore, here we investigated its effects on mitochondrial bioenergetic functions both in the dark and under photostimulation. Two experimental systems were utilized: (a) isolated rat liver mitochondria and (b) isolated perfused rat liver. Our data revealed that, independently of photostimulation, TBO presented affinity for mitochondria. Under photostimulation, TBO increased the protein carbonylation and lipid peroxidation levels (up to 109.40 and 119.87%, respectively) and decreased the reduced glutathione levels (59.72%) in mitochondria. TBO also uncoupled oxidative phosphorylation and photoinactivated the respiratory chain complexes I, II, and IV, as well as the F

Published

2022

2. The harmful acute effects of clomipramine in the rat liver: impairments in mitochondrial bioenergetics

Author

Paulo Francisco Veiga Bizerra, Fernanda Sayuri Itou da Silva, Eduardo Hideo Gilglioni, Letícia Fernanda Nanami, Eduardo Makiyama Klosowski, Byanca Thais Lima de Souza, Ana Flávia Gatto Raimundo, Karina Borba Paulino dos Santos, Juliana Moraes Mewes, Renato Polimeni Constantin, Márcio Shigueaki Mito, Emy Luiza Ishii-Iwamoto, Jorgete Constantin, Fábio Ermínio Mingatto, Giovana Natiele Machado Esquissato, Rogério Marchiosi, Wanderley Dantas dos Santos, Osvaldo Ferrarese-Filho, and Rodrigo Polimeni Constantin

Subjects

General Medicine, Toxicology

Published

2023

3. The metabolic and toxic acute effects of phloretin in the rat liver

Author

Fernanda Sayuri Itou da Silva, Paulo Francisco Veiga Bizerra, Márcio Shigueaki Mito, Renato Polimeni Constantin, Eduardo Makiyama Klosowski, Byanca Thais Lima de Souza, Paulo Vinicius Moreira da Costa Menezes, Paulo Sérgio Alves Bueno, Letícia Fernanda Nanami, Rogério Marchiosi, Wanderley Dantas dos Santos, Osvaldo Ferrarese-Filho, Emy Luiza Ishii-Iwamoto, and Rodrigo Polimeni Constantin

Subjects

Blood Glucose, Adenosine Triphosphate, Glucose, Liver, Phloretin, Gluconeogenesis, Animals, Mitochondria, Liver, General Medicine, Rats, Wistar, Toxicology, Rats

Abstract

The current study sought to evaluate the acute effects of phloretin (PH) on metabolic pathways involved in the maintenance of glycemia, specifically gluconeogenesis and glycogenolysis, in the perfused rat liver. The acute effects of PH on energy metabolism and toxicity parameters in isolated hepatocytes and mitochondria, as well as its effects on the activity of a few key enzymes, were also evaluated. PH inhibited gluconeogenesis from different substrates, stimulated glycogenolysis and glycolysis, and altered oxygen consumption. The citric acid cycle activity was inhibited by PH under gluconeogenic conditions. Similarly, PH reduced the cellular ATP/ADP and ATP/AMP ratios under gluconeogenic and glycogenolytic conditions. In isolated mitochondria, PH inhibited the electron transport chain and the F

Published

2022

4. The photosensitiser azure A disrupts mitochondrial bioenergetics through intrinsic and photodynamic effects

Author

Márcio Shigueaki Mito, Byanca Thais Lima de Souza, Renato Polimeni Constantin, Eduardo Hideo Gilglioni, Osvaldo Ferrarese-Filho, Karina Sayuri Utsunomiya, Eduardo Makiyama Klosowski, Paulo Cesar de Souza Pereira, Jorgete Constantin, Paulo Francisco Veiga Bizerra, Rodrigo Polimeni Constantin, Renato Sonchini Gonçalves, Wilker Caetano, Wanderley Dantas dos Santos, Rogério Marchiosi, Gislaine Cristiane Mantovanelli, Juliana Morais Mewes, Paulo Vinicius Moreira da Costa Menezes, Emy Luiza Ishii-Iwamoto, and Fernanda Sayuri Itou da Silva

Subjects

0301 basic medicine, Male, Bioenergetics, Cell Survival, Mitochondria, Liver, Oxidative phosphorylation, Mitochondrion, Toxicology, medicine.disease_cause, Azure Stains, Protein Carbonylation, 03 medical and health sciences, 0302 clinical medicine, Adenosine Triphosphate, Oxygen Consumption, medicine, Animals, Rats, Wistar, chemistry.chemical_classification, Reactive oxygen species, ATP synthase, biology, Cytosol, 030104 developmental biology, Mitochondrial respiratory chain, chemistry, Biochemistry, Liver, biology.protein, Hepatocytes, Lipid Peroxidation, Energy Metabolism, Reactive Oxygen Species, 030217 neurology & neurosurgery, Oxidative stress

Abstract

Azure A (AA) is a cationic molecule of the class of phenothiazines that has been applied in vitro as a photosensitising agent in photodynamic antimicrobial chemotherapy. It is a di-demethylated analogue of methylene blue (MB), which has been demonstrated to be intrinsically and photodynamically highly active on mitochondrial bioenergetics. However, as far as we know, there are no studies about the photodynamic effects of AA on mammalian mitochondria. Therefore, this investigation aimed to characterise the intrinsic and photodynamic acute effects of AA (0.5 40 μM) on isolated rat liver mitochondria, isolated hepatocytes, and isolated perfused rat liver. The effects of AA were assessed by evaluating several parameters of mitochondrial bioenergetics, oxidative stress, cell viability, and hepatic energy metabolism. The photodynamic effects of AA were assessed under simulated hypoxic conditions, a suitable way for mimicking the microenvironment of hypoxic solid tumour cells. AA interacted with the mitochondria and, upon photostimulation (10 min of light exposure), produced toxic amounts of reactive oxygen species (ROS), which damaged the organelle, as demonstrated by the high levels of lipid peroxidation and protein carbonylation. The photostimulated AA also depleted the GSH pool, which could compromise the mitochondrial antioxidant defence. Bioenergetically, AA photoinactivated the complexes I, II, and IV of the mitochondrial respiratory chain and the F1FO–ATP synthase complex, sharply inhibiting the oxidative phosphorylation. Upon photostimulation (10 min of light exposure), AA reduced the efficiency of mitochondrial energy transduction and oxidatively damaged lipids in isolated hepatocytes but did not decrease the viability of cells. Despite the useful photobiological properties, AA presented noticeable dark toxicity on mitochondrial bioenergetics, functioning predominantly as an uncoupler of oxidative phosphorylation. This harmful effect of AA was evidenced in isolated hepatocytes, in which AA diminished the cellular ATP content. In this case, the cells exhibited signs of cell viability reduction in the presence of high AA concentrations, but only after a long time of incubation (at least 90 min). The impairments on mitochondrial bioenergetics were also clearly manifested in intact perfused rat liver, in which AA diminished the cellular ATP content and stimulated the oxygen uptake. Consequently, gluconeogenesis and ureogenesis were strongly inhibited, whereas glycogenolysis and glycolysis were stimulated. AA also promoted the release of cytosolic and mitochondrial enzymes into the perfusate concomitantly with inhibition of oxygen consumption. In general, the intrinsic and photodynamic effects of AA were similar to those of MB, but AA caused some distinct effects such as the photoinactivation of the complex IV of the mitochondrial respiratory chain and a diminution of the ATP levels in the liver. It is evident that AA has the potential to be used in mitochondria-targeted photodynamic therapy, even under low oxygen concentrations. However, the fact that AA directly disrupts mitochondrial bioenergetics and affects several hepatic pathways that are linked to ATP metabolism, along with its ability to perturb cellular membranes and its little potential to reduce cell viability, could result in significant adverse effects especially in long-term treatments.

Published

2020

5. The photodynamic and direct actions of methylene blue on mitochondrial energy metabolism: A balance of the useful and harmful effects of this photosensitizer

Author

Paulo Vinicius Moreira da Costa Menezes, Karina Sayuri Utsunomiya, Márcio Shigueaki Mito, Paulo Francisco Veiga Bizerra, Gislaine Cristiane Mantovanelli, Rodrigo Polimeni Constantin, Renato Sonchini Gonçalves, Renato Polimeni Constantin, Wanderley Dantas dos Santos, Paulo Cesar de Souza Pereira, Osvaldo Ferrarese Filho, Jorgete Constantin, Emy Luiza Ishii-Iwamoto, Eduardo Hideo Gilglioni, Wilker Caetano, Eduardo Makiyama Klosowski, Juliana Morais Mewes, Rogério Marchiosi, and Byanca Thais Lima de Souza

Subjects

0301 basic medicine, Mitochondria, Liver, Oxidative phosphorylation, Mitochondrion, Biochemistry, Lipid peroxidation, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Physiology (medical), Animals, Photosensitizer, Glycolysis, Inner mitochondrial membrane, Photosensitizing Agents, ATP synthase, biology, Chemistry, Glutathione, Mitochondria, Rats, Methylene Blue, 030104 developmental biology, biology.protein, Biophysics, Energy Metabolism, 030217 neurology & neurosurgery

Abstract

According to the literature, methylene blue (MB) is a photosensitizer (PS) with a high affinity for mitochondria. Therefore, several studies have explored this feature to evaluate its photodynamic effects on the mitochondrial apoptotic pathway under normoxic conditions. We are aware only of limited reports regarding MB's photodynamic effects on mitochondrial energy metabolism, especially under hypoxic conditions. Thus, the purposes of this study were to determine the direct and photodynamic acute effects of MB on the energy metabolism of rat liver mitochondria under hypoxic conditions and its direct acute effects on several parameters linked to energy metabolism in the isolated perfused rat liver. MB presented a high affinity for mitochondria, irrespective of photostimulation or proton gradient formation. Upon photostimulation, MB demonstrated high in vitro oxidizing species generation ability. Consequently, MB damaged the mitochondrial macromolecules, as could be evidenced by the elevated levels of lipid peroxidation and protein carbonyls. In addition to generating a pro-oxidant environment, MB also led to a deficient antioxidant defence system, as indicated by the reduced glutathione (GSH) depletion. Bioenergetically, MB caused uncoupling of oxidative phosphorylation and led to photodynamic inactivation of complex I, complex II, and F1FO-ATP synthase complex, thus decreasing mitochondrial ATP generation. Contrary to what is expected for an ideal PS, MB displayed appreciable dark toxicity on mitochondrial energy metabolism. The results indicated that MB acted via at least three mechanisms: direct damage to the inner mitochondrial membrane; uncoupling of oxidative phosphorylation; and inhibition of electron transfer. Confirming the impairment of mitochondrial energy metabolism, MB also strongly inhibited mitochondrial ATP production. In the perfused rat liver, MB stimulated oxygen consumption, decreased the ATP/ADP ratio, inhibited gluconeogenesis and ureogenesis, and stimulated glycogenolysis, glycolysis, and ammoniagenesis, fully corroborating its uncoupling action in intact cells, as well. It can be concluded that even under hypoxic conditions, MB is a PS with potential for photodynamic effect-induced mitochondrial dysfunction. However, MB disrupts the mitochondrial energy metabolism even in the dark, causing energy-linked liver metabolic changes that could be harmful in specific circumstances.

Published

2020

6. The photodynamic and intrinsic effects of Azure B on mitochondrial bioenergetics and the consequences of its intrinsic effects on hepatic energy metabolism

Author

Paulo Vinicius Moreira da Costa Menezes, Rogério Marchiosi, Ana Flavia Gatto Raimundo, Wilker Caetano, Eduardo Makiyama Klosowski, Gislaine Cristiane Mantovanelli, Eduardo Hideo Gilglioni, Osvaldo Ferrarese-Filho, Jorgete Constantin, Renato Sonchini Gonçalves, Paulo Francisco Veiga Bizerra, Juliana Morais Mewes, Paulo Cesar de Souza Pereira, Wanderley Dantas dos Santos, Renato Polimeni Constantin, Byanca Thais Lima de Souza, Márcio Shigueaki Mito, Karina Sayuri Utsunomiya, Karina Borba Paulino dos Santos, Rodrigo Polimeni Constantin, and Emy Luiza Ishii-Iwamoto

Subjects

Bioenergetics, Biophysics, Dermatology, Oxidative phosphorylation, Mitochondrion, Azure Stains, chemistry.chemical_compound, Adenosine Triphosphate, medicine, Animals, Pharmacology (medical), Glycolysis, Rats, Wistar, Inner mitochondrial membrane, Photosensitizing Agents, ATP synthase, biology, Chemistry, Glutathione, medicine.disease, Mitochondria, Rats, Mitochondrial toxicity, Liver, Photochemotherapy, Oncology, Biochemistry, biology.protein, Energy Metabolism

Abstract

Background The present study aimed to characterize the intrinsic and photodynamic effects of azure B (AB) on mitochondrial bioenergetics, as well as the consequences of its intrinsic effects on hepatic energy metabolism. Methods Two experimental systems were utilized: (a) isolated rat liver mitochondria and (b) isolated perfused rat liver. Results AB interacted with mitochondria regardless of photostimulation, but its binding degree was reduced by mitochondrial energization. Under photostimulation, AB caused lipid peroxidation and protein carbonylation and decreased the content of reduced glutathione (GSH) in mitochondria. AB impaired mitochondrial bioenergetics in at least three distinct ways: (1) uncoupling of oxidative phosphorylation; (2) photoinactivation of complexes I and II; and (3) photoinactivation of the FoF1–ATP synthase complex. Without photostimulation, AB also demonstrated mitochondrial toxicity, which was characterized by the induction of lipid peroxidation, loss of inner mitochondrial membrane integrity, and uncoupling of oxidative phosphorylation. The perfused rat liver experiments showed that mitochondria were one of the major targets of AB, even in intact cells. AB inhibited gluconeogenesis and ureagenesis, two biosynthetic pathways strictly dependent on intramitochondrially generated ATP. Contrariwise, AB stimulated glycogenolysis and glycolysis, which are required compensatory pathways for the inhibited oxidative phosphorylation. Similarly, AB reduced the cellular ATP content and the ATP/ADP and ATP/AMP ratios. Conclusions Although the properties and severe photodynamic effects of AB on rat liver mitochondria might suggest its usefulness in PDT treatment of liver tumors, this possibility should be considered with precaution given the toxic intrinsic effects of AB on mitochondrial bioenergetics and energy-linked hepatic metabolism.

Published

2021

7. The Role of Mitochondria in Sex-Dependent Differences in Hepatic Steatosis and Oxidative Stress in Response to Cafeteria Diet-Induced Obesity in Mice

Author

Tiago Yoshida, Juliana Morais Mewes, Paulo Francisco Veiga Bizerra, Byanca Thais Lima de Souza, Fabiana Rodrigues Silva Gasparin, Eduardo Makiyama Klosowski, Rodrigo Polimeni Constantin, Gislaine Cristiane Mantovanelli, Maria Raquel Marçal Natali, Eduardo Hideo Gilglioni, Jorgete Constantin, Mariana Amâncio Daniel da Silva, Emy Luiza Ishii-Iwamoto, Márcio Shigueaki Mito, and Karina Sayuri Utsunomiya

Subjects

0301 basic medicine, Mitochondrial ROS, Male, medicine.medical_specialty, Antioxidant, medicine.medical_treatment, Mitochondria, Liver, lcsh:TX341-641, Mitochondrion, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Oxygen Consumption, cafeteria diet, Internal medicine, medicine, Animals, oxidative stress, Carbon Radioisotopes, Obesity, Animal Husbandry, Beta oxidation, chemistry.chemical_classification, Reactive oxygen species, Nutrition and Dietetics, Glutathione, Carbon Dioxide, medicine.disease, mitochondrial energy metabolism, Animal Feed, Diet, Fatty Liver, 030104 developmental biology, Endocrinology, chemistry, 030220 oncology & carcinogenesis, Female, Steatosis, ER stress, lcsh:Nutrition. Foods and food supply, Oxidative stress, Food Science

Abstract

Female mice fed a cafeteria diet (FCaf) develop higher liver steatosis and oxidative stress than males (MCaf) as a consequence of unresolved ER stress. Here, we investigated whether mitochondria play a role in this sex difference. The isolated mitochondria from FCaf showed more signs of oxidative stress than those of MCaf, correlated with a reduced content of GSH, increased amount of reactive oxygen species (ROS), and lower activities of enzymes involved in ROS neutralisation. Mitochondria from FCaf and MCaf livers exhibited lower rates of succinate-driven state III respiration and reduced ATPase activity in intact coupled mitochondria compared to their controls fed a standard diet (FC and MC), with no differences between the sexes. Fatty acid oxidation in mitochondria and peroxisomes was higher in MCaf and FCaf compared to their respective controls. In the intact perfused liver, there was no difference between sex or diet regarding the fatty acid oxidation rate. These results indicated that cafeteria diet did not affect mitochondrial energy metabolism, even in FCaf livers, which have higher steatosis and cellular oxidative stress. Nevertheless, the increase in mitochondrial ROS generation associated with a decrease in the antioxidant defence capacity, probably contributes to inducing or reinforcing the ER stress in FCaf livers.

Published

2019

8. CORANTES NATURAIS EXTRAÍDOS DE FRUTAS E HORTALIÇAS – UMA BREVE REVISÃO

Author

Jéssica Maria Ferreira de Almeida, Eduardo Makiyama Klosowski, Jéssica Barrionuevo Ressutte, and Grasiele Scaramal Madrona

Published

2019