Novel drug development opportunity for relaxin in acute myocardial infarction: evidences from a swine model

Perna, A. M.; Masini, Emanuela; Nistri, Silvia; Briganti, Vittorio; Chiappini, Laura; Stefàno, Pierluigi; Bigazzi, Mario; Pieroni, Cesco; Sacchi, Tatiana Bani; Bani, Danièle

doi:10.1096/fj.04-3664fje

Cited by 89 publications

(91 citation statements)

References 35 publications

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“…21 The anti-apoptotic effects of relaxin in the infarcted murine heart are also consistent with its effects in a porcine model of MI, 36 and its ability to protect cardiomyocytes from apoptosis in vitro; 16 while its pro-angiogenic Relaxin remodels post-infarct fibrotic healing CS Samuel et al effects are in keeping with that observed in the pig model of MI. 14 The rationale for Glut-1 staining was based on previous studies using endothelial expression of Glut-1 as a marker of active de novo capillary formation; where 75% of Glut-1 expression in the heart was localized to the capillary endothelium.…”

Section: Discussionsupporting

confidence: 56%

Relaxin remodels fibrotic healing following myocardial infarction

Samuel

Cendrawan

Gao

et al. 2011

Laboratory Investigation

101

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In the setting of myocardial infarction (MI), implanted stem cell viability is low and scar formation limits stem cell homing, viability, and integration. Thus, interventions that favorably remodel fibrotic healing may benefit stem cell therapies. However, it remains unclear whether it is feasible and safe to remodel fibrotic healing post-MI without compromising ventricular remodeling and dysfunction. This study, therefore, determined the anti-fibrotic and other effects of the hormone, relaxin in a mouse model of MI. Adult male mice underwent left coronary artery ligation-induced MI and were immediately treated with recombinant human relaxin (MI þ RLX) or vehicle (MI þ VEH) over 7 or 30 days, representing time points of early and mature fibrotic healing. Cardiac function was assessed by echocardiography and catheterization, while comprehensive immunohistochemistry, morphometry, and western blotting were performed to explore the relaxin-induced mechanisms of action post-MI. RLX significantly inhibited the MI-induced progression of cardiac fibrosis over 7 and 30 days, which was associated with a reduction in TGF-b1 expression, myofibroblast differentiation, and cardiomyocyte apoptosis in addition to a promotion of matrix metalloproteinase-13 levels and de novo blood vessel growth (all Po0.05 vs respective measurements from MI þ VEH mice). Despite the evident fibrotic healing post-MI, relaxin did not adversely affect the incidence of ventricular free-wall rupture or the extent of LV remodeling and dysfunction. These combined findings demonstrate that RLX favorably remodels the process of fibrotic healing post-infarction by lowering the density of mature scar tissue in the infarcted myocardium, border zone, and non-infarcted myocardium, and may, therefore, facilitate cell-based therapies in the setting of ischemic heart disease.

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Section: Discussionsupporting

confidence: 56%

Relaxin remodels fibrotic healing following myocardial infarction

Samuel

Cendrawan

Gao

et al. 2011

Laboratory Investigation

101

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“…The inhibition of either the nitric oxide pathway or glucocorticoid receptor stimulation significantly reduced the positive effects described previously for homogenous groups (10)(11)(12). Surprisingly for group 7 when we associated both inhibitors the severity that was developed although greater than for homogenous groups (6-7) was still less than that displayed by homogenous groups (3)(4) suggesting that there is another pathway involved in the treatment with relaxin.…”

Section: Pancreatic Edemamentioning

confidence: 55%

“…It has been reported that relaxin offers protection for reperfusion-induced cardiac injury increasing coronary blood flow favoring blood supply to the ischemic myocardium while it exerts a relaxant action on smooth muscle cells [10] . It has been shown that relaxin up regulates nitric oxide synthase (NOS) II expression thus inducing nitric oxide mediated vasodilatation by a controlled activation of endogenous nitric oxide biosynthesis [11] .…”

Section: R E L a X I N P R E V E N T S T H E D E V E L O P M E N T O mentioning

confidence: 99%

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Relaxin prevents the development of severe acute pancreatitis

Cosen-Binker¹,

Binker²,

Cosen³

et al. 2006

WJG

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AIM:To investigate the severity of acute pancreatitis (AP) is associated to the intensity of leukocyte activation, inflammatory up-regulation and microcirculatory disruption associated to ischemia-reperfusion injury. Microvascular integrity and inhibition of pro-infl ammatory mediators are key-factors in the evolution of AP. Relaxin is an insulin-like hormone that has been attributed vasorelaxant properties via the nitric oxide pathway while behaving as a glucocorticoid receptor agonist. METHODS:AP was induced by the bilio-pancreatic duct-outlet-exclusion closed-duodenal-loops model. Treatment with relaxin was done at different timepoints. Nitric oxide synthase inhibition by L-NAME and glucocorticoid receptor (GR) blockage by mifepristone was considered. AP severity was assessed by biochemical and histopathological analyses. RESULTS:Treatment with relaxin reduced serum amylase, lipase, C-reactive protein, IL-6, IL-10, hsp72, LDH and 8-isoprostane as well as pancreatic and lung myeloperoxidase. Acinar and fat necrosis, hemorrhage and neutrophil infiltrate were also decreased. ATP depletion and ADP/ATP ratio were reduced while caspases 2-3-8 and 9 activities were increased. L-NAME and mifepristone decreased the effi ciency of relaxin. CONCLUSION:Relaxin resulted beneficial in the treatment of AP combining the properties of a GR agonist

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“…This working hypothesis is based on the following mainstays: ( i ) blood vessels are a physiological target of RLX and their cells express the specific RLX receptor RXFP1 25; ( ii ) RLX up‐regulates NOS expression and nitric oxide production in vascular endothelial cells 26, 27, 28, 29, 30; ( iii ) RLX improves inflammation‐induced endothelial dysfunction and NOS fall 31, 32; and ( iv ) RLX reduces oxidative stress and nitric oxide failure in different animal models of vascular injury 33, 34, 35, 36, 37.…”

Section: Introductionmentioning

confidence: 99%

Protection from cigarette smoke‐induced vascular injury by recombinant human relaxin‐2 (serelaxin)

Pini

Boccalini

Baccari

et al. 2016

J Cellular Molecular Medi

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Smoking is regarded as a major risk factor for the development of cardiovascular diseases (CVD). This study investigates whether serelaxin (RLX, recombinant human relaxin‐2) endowed with promising therapeutic properties in CVD, can be credited of a protective effect against cigarette smoke (CS)‐induced vascular damage and dysfunction. Guinea pigs exposed daily to CS for 8 weeks were treated with vehicle or RLX, delivered by osmotic pumps at daily doses of 1 or 10 μg. Controls were non‐smoking animals. Other studies were performed on primary guinea pig aortic endothelial (GPAE) cells, challenged with CS extracts (CSE) in the absence and presence of 100 ng/ml (17 nmol/l) RLX. In aortic specimens from CS‐exposed guinea pigs, both the contractile and the relaxant responses to phenylephrine and acetylcholine, respectively, were significantly reduced in amplitude and delayed, in keeping with the observed adverse remodelling of the aortic wall, endothelial injury and endothelial nitric oxide synthase (eNOS) down‐regulation. RLX at both doses maintained the aortic contractile and relaxant responses to a control‐like pattern and counteracted aortic wall remodelling and endothelial derangement. The experiments with GPAE cells showed that CSE significantly decreased cell viability and eNOS expression and promoted apoptosis by sparkling oxygen free radical‐related cytotoxicity, while RLX counterbalanced the adverse effects of CSE. These findings demonstrate that RLX is capable of counteracting CS‐mediated vascular damage and dysfunction by reducing oxidative stress, thus adding a tile to the growing mosaic of the beneficial effects of RLX in CVD.

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Novel drug development opportunity for relaxin in acute myocardial infarction: evidences from a swine model

Cited by 89 publications

References 35 publications

Relaxin remodels fibrotic healing following myocardial infarction

Relaxin remodels fibrotic healing following myocardial infarction

Relaxin prevents the development of severe acute pancreatitis

Protection from cigarette smoke‐induced vascular injury by recombinant human relaxin‐2 (serelaxin)

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