The Biological Effects of Ivabradine in Cardiovascular Disease

Speranza, Lorenza; Franceschelli, Sara; Riccioni, Graziano

doi:10.3390/molecules17054924

Cited by 26 publications

(15 citation statements)

References 62 publications

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“…As shown in Figure 1A-C, the monocytes from pretreatment patients showed the activation of the TAK-1 and of the IKKbeta by phosphorylation on these sites, whereas un-phosphorylated TAK-1 and IKKbeta levels did not change after treatment. As expected, the level of pIkBalpha (Ser-32) is higher in pre-treated patients CCL5 -1.8±0.6 (1) −2.1±0.4 (3) CD14 -1.8±0.5 (1) −1.7±0.3 (4) ITGAM -2±0.6 (1) −2.3±0.5 (4) CCR1 -2.8±0.7 (2) −3.8±0.9 (3) NFKBIA 2.5±0.6 (1) 2.2±0.2 (3) PTPN6 1.9±0.6 (2) 2.4±0.3 (4) TNFAIP3 3±0.9 (1) 3.6±1.1 (3) CCL5 Protein 3., (1) FDR: 0%, (2) FDR: 0.1% (n=11); (3) p<.01, (4) p<.05 (n=50) © 1996-2017 with conventional drugs, whereas the WB analysis for un-phosphorylated IkBalpha protein confirmed an up-regulation of the mRNA reported through Microarray analysis as well as the qPCR analysis after therapy. As a post-translational modification of the NF-kB (p65) affecting its transcriptional activities, we performed further studies to determine the phosphorylation of the p65 at Ser-536 by the WB, using specific phospho-p65 antibody on nuclear protein extracts.…”

Section: Tak-1/ikk/nf-kb Signaling In Monocytes Of Achf Patientssupporting

confidence: 80%

“…Heart Failure (HF) is one of the most common pathological condition in the Western World having the highest impact on survival and on the quality of life of patients. Although there have been significant progress that have reduced the mortality rate of the disease or delayed its progression and made way for quality of life considered acceptable, the prognosis of HF remains poor (1)(2)(3). Progression of HF is a result of compensatory mechanisms and modulation of T cells and complement system, and activation of a variety of pro-inflammatory cytokines, such as Tumor Necrosis Factor (TNF)-α and Interleukin (IL)-6 (4)(5)(6)(7)(8).…”

Section: Introductionmentioning

confidence: 99%

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The NF-kB regulates the SHP-1 expression in monocytes in congestive heart failure

Pesce

Franceschelli²,

Ferrone

et al. 2017

Front Biosci

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It has been shown that functional recovery of patients with acute congestive heart failure (ACHF) after treatment with conventional drugs (CD) is mediated by suppression of inflammation in peripheral blood mononuclear cells. Here, we analyzed gene expression profiles of monocytes from symptomatic ACHF patients (NYHA Class III-IV) before and after pharmacological treatment with CD. The treatment was associated with selective down-regulation of "TNFR signaling" and pro-inflammatory mediators CCL5, MIP-1α receptor, CD14, ITGAM, and significant up-regulation of "TNFR signaling" as evidenced by increase in anti-inflammatory factors including NF-kBIA, TNFAIP3 and SHP-1. In monocyte TNF-alpha-stimulated there is a down-regulation of the phosphatase SHP-1 which induces a significant activation of TAK-1/IKK/NF-kB signaling. These findings suggest that the therapeutic impact of CD treatment in symptomatic ACHF includes negative regulation of the NF-kB signaling in monocytes and the improvement of the SHP-1 activity.

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Section: Tak-1/ikk/nf-kb Signaling In Monocytes Of Achf Patientssupporting

confidence: 80%

Section: Introductionmentioning

confidence: 99%

The NF-kB regulates the SHP-1 expression in monocytes in congestive heart failure

Pesce

Franceschelli²,

Ferrone

et al. 2017

Front Biosci

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“…Inflammation is a major condition associated with various diseases and is a natural host defensive response to invading pathogens and tissue injury with the involvement of phagocytic cells such as macrophages, mast cells, dendritic cells, granulocytes, and innate lymphocytes (Speranza et al, ; Pesce et al, ). In many cases, inflammation is demonstrated to be an important contributor to diseases such as cancer, diabetes, and cardiovascular diseases (Speranza et al, ; Khuda‐Bukhsh et al, ). The Silent Information Regulator‐1 (Sirtuin1, SIRT‐1), a member of NAD + dependent class III histone deacetylase, has been shown to be involved in a variety of pathophysiological processes, such as inflammation, the modulation of cell growth and metabolism, and carcinogenesis.…”

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confidence: 99%

A Novel Biological Role of α-Mangostin in Modulating Inflammatory Response Through the Activation of SIRT-1 Signaling Pathway

et al. 2016

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Several studies have shown that xanthones obtained from Garcinia Mangostana (GM) have remarkable biological activities. α-mangostin (α-MG) is the main constituent of the fruit hull of the GM. Several findings have suggested that SIRT-1, a nuclear histone deacetylase, could influence cellular function by the inhibition of NF-kB signaling. ROS can inhibit SIRT-1 activity by initiating oxidative modifications on its cysteine residues, and suppression of SIRT-1 enhances the NF-κB signaling resulting in inflammatory responses. The goals of the present study were to evaluate the quantity of α-MG in the methanolic extract of GM (Vithagroup Spa) and to investigate the activity of this xanthone in U937 cell line and in human monocytes from responsive to inflammatory insult analyzing the possible changes on the activation of SIRT-1 protein via NF-Kb. Cells were treated with the methanolic extract of GM and/or LPS. The chromatographic separation of α-MG was performed by an HPLC analysis. EX 527, a specific SIRT-1 inhibitor, was used to determine if SIRT-1/NfkB signaling pathway might be involved in α-MG action on cells. Our results show that α-MG inhibits p65 acetylation and down-regulates the pro-inflammatory gene products as COX-2, iNOS via SIRT-1 activation. Cells treated with EX 527 showed an up-regulation of NFkB acetylation and an over expression of inducible enzymes and their product of catalysis (NO and PGE2). These results suggest that α-MG may be useful for the development of alternative pharmacological strategies aimed at reducing the inflammatory process. J. Cell. Physiol. 231: 2439-2451, 2016. © 2016 Wiley Periodicals, Inc.

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“…These effects can improve endothelial function, modulate immune cells and enhance a long-term adaptation in calcium handling. [ 120 ] In a dystrophy case report, ivabradine normalizes sinus tachycardia and heart failure in Becker’s muscular dystrophy patients with dilated cardiomyopathy and reduces arrhythmic events and left ventricular remodeling. [ 121 ]…”

Section: Treatmentsmentioning

confidence: 99%

Inflammation and cardiac dysfunction during sepsis, muscular dystrophy, and myocarditis

Liu

Peng

et al. 2013

Burn Trauma

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Inflammation plays an important role in cardiac dysfunction under different situations. Acute systemic inflammation occurring in patients with severe burns, trauma, and inflammatory diseases causes cardiac dysfunction, which is one of the leading causes of mortality in these patients. Acute sepsis decreases cardiac contractility and impairs myocardial compliance. Chronic inflammation such as that occurring in Duchenne muscular dystropshy and myocarditis may cause adverse cardiac remodeling including myocyte hypertrophy and death, fibrosis, and altered myocyte function. However, the underlying cellular and molecular mechanisms for inflammatory cardiomyopathy are still controversial probably due to multiple factors involved. Potential mechanisms include the change in circulating blood volume; a direct inhibition of myocyte contractility by cytokines (tumor necrosis factor (TNF)-α, interleukin (IL)-1β); abnormal nitric oxide and reactive oxygen species (ROS) signaling; mitochondrial dysfunction; abnormal excitation-contraction coupling; and reduced calcium sensitivity at the myofibrillar level and blunted β-adrenergic signaling. This review will summarize recent advances in diagnostic technology, mechanisms, and potential therapeutic strategies for inflammation-induced cardiac dysfunction.

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The Biological Effects of Ivabradine in Cardiovascular Disease

Cited by 26 publications

References 62 publications

The NF-kB regulates the SHP-1 expression in monocytes in congestive heart failure

The NF-kB regulates the SHP-1 expression in monocytes in congestive heart failure

A Novel Biological Role of α-Mangostin in Modulating Inflammatory Response Through the Activation of SIRT-1 Signaling Pathway

Inflammation and cardiac dysfunction during sepsis, muscular dystrophy, and myocarditis

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