Your search keyword '"Tamás Baranyai"' showing total 62 results

51. Author Correction: MicroRNA interactome analysis predicts post-transcriptional regulation of ADRB2 and PPP3R1 in the hypercholesterolemic myocardium.

Author

Ágg, Bence, Baranyai, Tamás, Makkos, András, Vető, Borbála, Faragó, Nóra, Zvara, Ágnes, Giricz, Zoltán, Veres, Dániel V., Csermely, Péter, Arányi, Tamás, Puskás, László G., Varga, Zoltán V., and Ferdinandy, Péter

Abstract

A correction to this article has been published and is linked from the HTML and PDF versions of this paper. The error has not been fixed in the paper. [ABSTRACT FROM AUTHOR]

Published

2018

52. Selegiline reduces adiposity induced by high-fat, high-sucrose diet in male rats.

Author

Nagy, Csilla Terézia, Koncsos, Gábor, Varga, Zoltán V., Baranyai, Tamás, Tuza, Sebestyén, Kassai, Ferenc, Ernyey, Aliz Judit, Gyertyán, István, Király, Kornél, Oláh, Attila, Radovits, Tamás, Merkely, Béla, Bukosza, Nóra, Szénási, Gábor, Hamar, Péter, Mathé, Domokos, Szigeti, Krisztián, Pelyhe, Csilla, Jelemenský, Marek, and Onódi, Zsófia

Subjects

SELEGILINE, OBESITY, HIGH-carbohydrate diet, HIGH-fat diet, WEIGHT loss

Abstract

Background and Purpose: Incidence and severity of obesity are increasing worldwide, however, efficient and safe pharmacological treatments are not yet available. Certain MAO inhibitors reduce body weight, although their effects on metabolic parameters have not been investigated. Here, we have assessed effects of a widely used, selective MAO-B inhibitor, selegiline, on metabolic parameters in a rat model of diet-induced obesity.Experimental Approach: Male Long-Evans rats were given control (CON) or a high-fat (20%), high-sucrose (15%) diet (HFS) for 25 weeks. From week 16, animals were injected s.c. with 0.25 mg·kg-1 selegiline (CON + S and HFS + S) or vehicle (CON, HFS) once daily. Whole body, subcutaneous and visceral fat was measured by CT, and glucose and insulin tolerance were tested. Expression of glucose transporters and chemokines was assessed by quantitative RT-PCR.Key Results: Selegiline decreased whole body fat, subcutaneous- and visceral adiposity, measured by CT and epididymal fat weight in the HFS group, compared with HFS placebo animals, without influencing body weight. Oral glucose tolerance and insulin tolerance tests showed impaired glucose homeostasis in HFS and HFS + S groups, although insulin levels in plasma and pancreas were unchanged. HFS induced expression of Srebp-1c, Glut1 and Ccl3 in adipose tissue, which were alleviated by selegiline.Conclusions and Implications: Selegiline reduced adiposity, changes in adipose tissue energy metabolism and adipose inflammation induced by HFS diet without affecting the increased body weight, impairment of glucose homeostasis, or behaviour. These results suggest that selegiline could mitigate harmful effects of visceral adiposity. [ABSTRACT FROM AUTHOR]

Published

2018

53. Alternative Splicing of NOX4 in the Failing Human Heart.

Author

Varga, Zoltán V., Pipicz, Márton, Baán, Júlia A., Baranyai, Tamás, Koncsos, Gábor, Leszek, Przemyslaw, Kuśmierczyk, Mariusz, Sánchez-Cabo, Fátima, García-Pavía, Pablo, Brenner, Gábor J., Giricz, Zoltán, Csont, Tamás, Mendler, Luca, Lara-Pezzi, Enrique, Pacher, Pál, and Ferdinandy, Péter

Subjects

NADPH oxidase, RNA splicing, HEART failure, OXIDATIVE stress, ISOENZYMES, RNA sequencing

Abstract

Increased oxidative stress is a major contributor to the development and progression of heart failure, however, our knowledge on the role of the distinct NADPH oxidase (NOX) isoenzymes, especially on NOX4 is controversial. Therefore, we aimed to characterize NOX4 expression in human samples from healthy and failing hearts. Explanted human heart samples (left and right ventricular, and septal regions) were obtained from patients suffering from heart failure of ischemic or dilated origin. Control samples were obtained from donor hearts that were not used for transplantation. Deep RNA sequencing of the cardiac transcriptome indicated extensive alternative splicing of the NOX4 gene in heart failure as compared to samples from healthy donor hearts. Long distance PCR analysis with a universal 5'-3' end primer pair, allowing amplification of different splice variants, confirmed the presence of the splice variants. To assess translation of the alternatively spliced transcripts we determined protein expression of NOX4 by using a specific antibody recognizing a conserved region in all variants. Western blot analysis showed up-regulation of the full-length NOX4 in ischemic cardiomyopathy samples and confirmed presence of shorter isoforms both in control and failing samples with disease-associated expression pattern. We describe here for the first time that NOX4 undergoes extensive alternative splicing in human hearts which gives rise to the expression of different enzyme isoforms. The full length NOX4 is significantly upregulated in ischemic cardiomyopathy suggesting a role for NOX4 in ROS production during heart failure. [ABSTRACT FROM AUTHOR]

Published

2017

54. In vivo MRI and ex vivo histological assessment of the cardioprotection induced by ischemic preconditioning, postconditioning and remote conditioning in a closed-chest porcine model of reperfused acute myocardial infarction: importance of microvasculature.

Author

Baranyai, Tamás, Giricz, Zoltán, Varga, Zoltán V., Koncsos, Gábor, Lukovic, Dominika, Makkos, András, Sárközy, Márta, Pávó, Noémi, Jakab, András, Czimbalmos, Csilla, Vágó, Hajnalka, Ruzsa, Zoltán, Tóth, Levente, Garamvölgyi, Rita, Merkely, Béla, Schulz, Rainer, Gyöngyösi, Mariann, and Ferdinandy, Péter

Subjects

ISCHEMIA diagnosis, MYOCARDIAL infarction diagnosis, CARDIOTONIC agents, CARDIAC magnetic resonance imaging, NECROSIS, CLINICAL trials, ANIMAL experimentation, BLOOD vessels, CORONARY disease, EDEMA, ELECTROCARDIOGRAPHY, HEART function tests, HEMODYNAMICS, MAGNETIC resonance imaging, MYOCARDIAL reperfusion complications, STAINS & staining (Microscopy), SWINE, THERAPEUTICS, DIAGNOSIS

Abstract

Background: Cardioprotective value of ischemic post- (IPostC), remote (RIC) conditioning in acute myocardial infarction (AMI) is unclear in clinical trials. To evaluate cardioprotection, most translational animal studies and clinical trials utilize necrotic tissue referred to the area at risk (AAR) by magnetic resonance imaging (MRI). However, determination of AAR by MRI' may not be accurate, since MRI-indices of microvascular damage, i.e., myocardial edema and microvascular obstruction (MVO), may be affected by cardioprotection independently from myocardial necrosis. Therefore, we assessed the effect of IPostC, RIC conditioning and ischemic preconditioning (IPreC; positive control) on myocardial necrosis, edema and MVO in a clinically relevant, closed-chest pig model of AMI.Methods and Results: Acute myocardial infarction was induced by a 90-min balloon occlusion of the left anterior descending coronary artery (LAD) in domestic juvenile female pigs. IPostC (6 × 30 s ischemia/reperfusion after 90-min occlusion) and RIC (4 × 5 min hind limb ischemia/reperfusion during 90-min LAD occlusion) did not reduce myocardial necrosis as assessed by late gadolinium enhancement 3 days after reperfusion and by ex vivo triphenyltetrazolium chloride staining 3 h after reperfusion, however, the positive control, IPreC (3 × 5 min ischemia/reperfusion before 90-min LAD occlusion) did. IPostC and RIC attenuated myocardial edema as measured by cardiac T2-weighted MRI 3 days after reperfusion, however, AAR measured by Evans blue staining was not different among groups, which confirms that myocardial edema is not a measure of AAR, IPostC and IPreC but not RIC decreased MVO.Conclusion: We conclude that IPostC and RIC interventions may protect the coronary microvasculature even without reducing myocardial necrosis. [ABSTRACT FROM AUTHOR]

Published

2017

55. Diastolic dysfunction in prediabetic male rats: Role of mitochondrial oxidative stress.

Author

Koncsos, Gábor, Varga, Zoltán V., Baranyai, Tamás, Boengler, Kerstin, Rohrbach, Susanne, Ling Li, Schlüter, Klaus-Dieter, Schreckenberg, Rolf, Radovits, Tamás, Oláh, Attila, Mátyás, Csaba, Lux, Árpád, Al-Khrasani, Mahmoud, Komlódi, Tímea, Bukosza, Nóra, Máthé, Domokos, Deres, László, Barteková, Monika, Rajtík, Tomáš, and Adameová, Adriana

Subjects

DIASTOLE (Cardiac cycle), PREDIABETIC state, OXIDATIVE stress

Abstract

Although incidence and prevalence of prediabetes are increasing, little is known about its cardiac effects. Therefore, our aim was to investigate the effect of prediabetes on cardiac function and to characterize parameters and pathways associated with deteriorated cardiac performance. Long-Evans rats were fed with either control or high-fat chow for 21 wk and treated with a single low dose (20 mg/kg) of streptozotocin at week 4. High-fat and streptozotocin treatment induced prediabetes as characterized by slightly elevated fasting blood glucose, impaired glucose and insulin tolerance, increased visceral adipose tissue and plasma leptin levels, as well as sensory neuropathy. In prediabetic animals, a mild diastolic dysfunction was observed, the number of myocardial lipid droplets increased, and left ventricular mass and wall thickness were elevated; however, no molecular sign of fibrosis or cardiac hypertrophy was shown. In prediabetes, production of reactive oxygen species was elevated in subsarcolemmal mitochondria. Expression of mitofusin-2 was increased, while the phosphorylation of phospholamban and expression of Bcl-2/adenovirus E1B 19-kDa protein- interacting protein 3 (BNIP3, a marker of mitophagy) decreased. However, expression of other markers of cardiac auto- and mitophagy, mitochondrial dynamics, inflammation, heat shock proteins, Ca2+/calmodulin-dependent protein kinase II, mammalian target of rapamycin, or apoptotic pathways were unchanged in prediabetes. This is the first comprehensive analysis of cardiac effects of prediabetes indicating that mild diastolic dysfunction and cardiac hypertrophy are multifactorial phenomena that are associated with early changes in mitophagy, cardiac lipid accumulation, and elevated oxidative stress and that prediabetes-induced oxidative stress originates from the subsarcolemmal mitochondria. [ABSTRACT FROM AUTHOR]

Published

2016

56. Myostatin and IGF-I signaling in end-stage human heart failure: a qRT-PCR study.

Author

Baán, Júlia Aliz, Varga, Zoltán V., Leszek, Przemyslaw, Kuśmierczyk, Mariusz, Baranyai, Tamás, Dux, László, Ferdinandy, Péter, Braun, Thomas, and Mendler, Luca

Subjects

MYOSTATIN, HEART failure, TRANSFORMING growth factors-beta, HEART diseases, HEART cells, ACTIVIN, GLYCOPROTEINS

Abstract

Background Myostatin (Mstn) is a key regulator of heart metabolism and cardiomyocyte growth interacting tightly with insulin-like growth factor (IGF-I) under physiological conditions. The pathological role of Mstn has also been suggested since Mstn protein was shown to be upregulated in the myocardium of end-stage heart failure. However, no data are available about the regulation of gene expression of Mstn and IGF-I in different regions of healthy or pathologic human hearts, although they both might play a crucial role in the pathomechanism of heart failure. Methods In the present study, heart samples were collected from left ventricles, septum and right ventricles of control healthy individuals as well as from failing hearts of dilated (DCM) or ischemic cardiomyopathic (ICM) patients. A comprehensive qRT-PCR analysis of Mstn and IGF-I signaling was carried out by measuring expression of Mstn, its receptor Activin receptor IIB (ActRIIB), IGF-I, IGF-I receptor (IGF-IR), and the negative regulator of Mstn miR-208, respectively. Moreover, we combined the measured transcript levels and created complex parameters characterizing either Mstn- or IGF-I signaling in the different regions of healthy or failing hearts. Results We have found that in healthy control hearts, the ratio of Mstn/IGF-I signaling was significantly higher in the left ventricle/septum than in the right ventricle. Moreover, Mstn transcript levels were significantly upregulated in all heart regions of DCM but not ICM patients. However, the ratio of Mstn/IGF-I signaling remained increased in the left ventricle/septum compared to the right ventricle of DCM patients (similarly to the healthy hearts). In contrast, in ICM hearts significant transcript changes were detected mainly in IGFI signaling. In paralell with these results miR-208 showed mild upregulation in the left ventricle of both DCM and ICM hearts. Conclusions This is the first demonstration of a spatial asymmetry in the expression pattern of Mstn/IGF-I in healthy hearts, which is likely to play a role in the different growth regulation of left vs. right ventricle. Moreover, we identified Mstn as a massively regulated gene in DCM but not in ICM as part of possible compensatory mechanisms in the failing heart. [ABSTRACT FROM AUTHOR]

Published

2015

57. MicroRNA interactome analysis predicts post-transcriptional regulation of ADRB2 and PPP3R1 in the hypercholesterolemic myocardium

Author

Ágg, Bence, Baranyai, Tamás, Makkos, András, Vető, Borbála, Faragó, Nóra, Zvara, Ágnes, Giricz, Zoltán, Veres, Dániel V., Csermely, Péter, Arányi, Tamás, Puskás, László G., Varga, Zoltán V., and Ferdinandy, Péter

Published

2018

58. Acknowledgment to Reviewers of JCM in 2021.

Subjects

SCHOLARLY publishing

Published

2022

59. Hidden Cardiotoxicity of Rofecoxib Can be Revealed in Experimental Models of Ischemia/Reperfusion.

Author

Brenner, Gábor B., Makkos, András, Nagy, Csilla Terézia, Onódi, Zsófia, Sayour, Nabil V., Gergely, Tamás G., Kiss, Bernadett, Görbe, Anikó, Sághy, Éva, Zádori, Zoltán S., Lázár, Bernadette, Baranyai, Tamás, Varga, Richárd S., Husti, Zoltán, Varró, András, Tóthfalusi, László, Schulz, Rainer, Baczkó, István, Giricz, Zoltán, and Ferdinandy, Péter

Subjects

MYOCARDIAL reperfusion, ROFECOXIB, CARDIOTOXICITY, CLINICAL drug trials, VENTRICULAR fibrillation, REPERFUSION

Abstract

Cardiac adverse effects are among the leading causes of the discontinuation of clinical trials and the withdrawal of drugs from the market. The novel concept of 'hidden cardiotoxicity' is defined as cardiotoxicity of a drug that manifests in the diseased (e.g., ischemic/reperfused), but not in the healthy heart or as a drug-induced deterioration of cardiac stress adaptation (e.g., ischemic conditioning). Here, we aimed to test if the cardiotoxicity of a selective COX-2 inhibitor rofecoxib that was revealed during its clinical use, i.e., increased occurrence of proarrhythmic and thrombotic events, could have been revealed in early phases of drug development by using preclinical models of ischemia/reperfusion (I/R) injury. Rats that were treated with rofecoxib or vehicle for four weeks were subjected to 30 min. coronary artery occlusion and 120 min. reperfusion with or without cardioprotection that is induced by ischemic preconditioning (IPC). Rofecoxib increased overall the arrhythmias including ventricular fibrillation (VF) during I/R. The proarrhythmic effect of rofecoxib during I/R was not observed in the IPC group. Rofecoxib prolonged the action potential duration (APD) in isolated papillary muscles, which was not seen in the simulated IPC group. Interestingly, while showing hidden cardiotoxicity manifested as a proarrhythmic effect during I/R, rofecoxib decreased the infarct size and increased the survival of adult rat cardiac myocytes that were subjected to simulated I/R injury. This is the first demonstration that rofecoxib increased acute mortality due to its proarrhythmic effect via increased APD during I/R. Rofecoxib did not interfere with the cardiprotective effect of IPC; moreover, IPC was able to protect against rofecoxib-induced hidden cardiotoxicity. These results show that cardiac safety testing with simple preclinical models of I/R injury uncovers hidden cardiotoxicity of rofecoxib and might reveal the hidden cardiotoxicity of other drugs. [ABSTRACT FROM AUTHOR]

Published

2020

60. Glomerular Collagen Deposition and Lipocalin-2 Expression Are Early Signs of Renal Injury in Prediabetic Obese Rats.

Author

Bukosza, Eva Nora, Kaucsár, Tamás, Godó, Mária, Lajtár, Enikő, Tod, Pál, Koncsos, Gábor, Varga, Zoltán V., Baranyai, Tamás, Tu, Nguyen Minh, Schachner, Helga, Sőti, Csaba, Ferdinandy, Péter, Giricz, Zoltán, Szénási, Gábor, and Hamar, Péter

Abstract

Feeding rats with high-fat diet (HFD) with a single streptozotocin (STZ) injection induced obesity, slightly elevated fasting blood glucose and impaired glucose and insulin tolerance, and caused cardiac hypertrophy and mild diastolic dysfunction as published before by Koncsos et al. in 2016. Here we aimed to explore the renal consequences in the same groups of rats. Male Long-Evans rats were fed normal chow (CON; n = 9) or HFD containing 40% lard and were administered STZ at 20 mg/kg (i.p.) at week four (prediabetic rats, PRED, n = 9). At week 21 blood and urine samples were taken and kidney and liver samples were collected for histology, immunohistochemistry and for analysis of gene expression. HFD and STZ increased body weight and visceral adiposity and plasma leptin concentration. Despite hyperleptinemia, plasma C-reactive protein concentration decreased in PRED rats. Immunohistochemistry revealed elevated collagen IV protein expression in the glomeruli, and Lcn2 mRNA expression increased, while Il-1β mRNA expression decreased in both the renal cortex and medulla in PRED vs. CON rats. Kidney histology, urinary protein excretion, plasma creatinine, glomerular Feret diameter, desmin protein expression, and cortical and medullary mRNA expression of TGF-β1, Nrf2, and PPARγ were similar in CON and PRED rats. Reduced AMPKα phosphorylation of the autophagy regulator Akt was the first sign of liver damage, while plasma lipid and liver enzyme concentrations were similar. In conclusion, glomerular collagen deposition and increased lipocalin-2 expression were the early signs of kidney injury, while most biomarkers of inflammation, oxidative stress and fibrosis were negative in the kidneys of obese, prediabetic rats with mild heart and liver injury. [ABSTRACT FROM AUTHOR]

Published

2019

61. Transcriptional Alterations by Ischaemic Postconditioning in a Pig Infarction Model: Impact on Microvascular Protection.

Author

Lukovic, Dominika, Gugerell, Alfred, Zlabinger, Katrin, Winkler, Johannes, Pavo, Noemi, Baranyai, Tamás, Giricz, Zoltán, Varga, Zoltán V., Riesenhuber, Martin, Spannbauer, Andreas, Traxler, Denise, Jakab, András, Garamvölgyi, Rita, Petnehazy, Örs, Pils, Dietmar, Tóth, Levente, Schulz, Rainer, Ferdinandy, Péter, and Gyöngyösi, Mariann

Subjects

ANIMAL models of myocardial infarction, PERCUTANEOUS coronary intervention, TRANSCRIPTOMES, CELL proliferation, CELL adhesion

Abstract

Although the application of cardioprotective ischaemia/reperfusion (I/R) stimuli after myocardial infarction (MI) is a promising concept for salvaging the myocardium, translation to a clinical scenario has not fulfilled expectations. We have previously shown that in pigs, ischaemic postconditioning (IPostC) reduces myocardial oedema and microvascular obstruction (MVO), without influencing myocardial infarct size. In the present study, we analyzed the mechanisms underlying the IPostC-induced microvascular protection by transcriptomic analysis, followed by pathway analysis. Closed-chest reperfused MI was induced by 90 min percutaneous balloon occlusion of the left anterior descending coronary artery, followed by balloon deflation in anaesthetised pigs. Animals were randomised to IPostC (n = 8), MI (non-conditioned, n = 8), or Control (sham-operated, n = 4) groups. After three hours or three days follow-up, myocardial tissue samples were harvested and subjected to RNA-seq analysis. Although the transcriptome analysis revealed similar expression between IPostC and MI in transcripts involved in cardioprotective pathways, we identified gene expression changes responding to IPostC at the three days follow-up. Focal adhesion signaling, downregulated genes participating in cardiomyopathy and activation of blood cells may have critical consequences for microvascular protection. Specific analyses of the gene subsets enriched in the endothelium of the infarcted area, revealed strong deregulation of transcriptional functional clusters, DNA processing, replication and repair, cell proliferation, and focal adhesion, suggesting sustentative function in the endothelial cell layer protection and integrity. The spatial and time-dependent transcriptome analysis of porcine myocardium supports a protective effect of IPostC on coronary microvasculature post-MI. [ABSTRACT FROM AUTHOR]

Published

2019

62. Errata: Patients with Moderate Non-Culprit Coronary Lesions of Recent Acute Coronary Syndrome: A Comparison of Fractional Flow Reserve and Dobutamine Stress Echocardiography.

Subjects

Humans, Echocardiography, Stress, Dobutamine, Coronary Angiography, Fractional Flow Reserve, Myocardial, Acute Coronary Syndrome diagnostic imaging

Abstract

An error appeared in the article entitled "Patients with Moderate Non-Culprit Coronary Lesions of Recent Acute Coronary Syndrome: A Comparison of Fractional Flow Reserve and Dobutamine Stress Echocardiography" by Abdelkrim Ahres, Balázs Jablonkai, Ágnes Schrancz, Zsuzsanna Balogh, Andrea Kenessey, Tamás Baranyai, Ágnes Őze, Zsolt Szigeti, Gábor Rubóczky, Béla Nagybaczoni, Astrid Apor, Judit Simon, Bálint Szilveszter, Márton Kolossváry, Béla Merkely, Pál Maurovich-Horvat, and Péter Andrássy (Vol. 62 No.5, 952-961, 2021). The affiliation of the first author on page 952 should be replaced by the following.

Published

2023