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

Pini, Alessandro; Boccalini, Giulia; Baccari, Maria Caterina; Becatti, Matteo; Garella, Rachele; Fiorillo, Claudia; Calosi, Laura; Bani, Danièle; Nistri, Silvia

doi:10.1111/jcmm.12802

Cited by 34 publications

(28 citation statements)

References 58 publications

(97 reference statements)

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“…Encouraging results from both cell and animal studies support further development and clinical evaluation of relaxin-2 as a first-in-kind therapy for arthrofibroses. the heart, lungs, kidney, and liver (30)(31)(32)(33)(34)(35). Our proposal stems from anecdotal clinical observation among a cohort of arthrofibrosis-afflicted female patients who experienced lasting motion restoration and reduced joint pain during and after pregnancy (E.K.R.).…”

Section: Significancementioning

confidence: 99%

Intraarticular injection of relaxin-2 alleviates shoulder arthrofibrosis

Blessing

Okajima

Cubria

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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Arthrofibrosis is a prevalent condition affecting greater than 5% of the general population and leads to a painful decrease in joint range of motion (ROM) and loss of independence due to pathologic accumulation of periarticular scar tissue. Current treatment options are limited in effectiveness and do not address the underlying cause of the condition: accumulation of fibrotic collagenous tissue. Herein, the naturally occurring peptide hormone relaxin-2 is administered for the treatment of adhesive capsulitis (frozen shoulder) and to restore glenohumeral ROM in shoulder arthrofibrosis. Recombinant human relaxin-2 down-regulates type I collagen and α smooth muscle actin production and increases intracellular cAMP concentration in human fibroblast-like synoviocytes, consistent with a mechanism of extracellular matrix degradation and remodeling. Pharmacokinetic profiling of a bolus administration into the glenohumeral joint space reveals the brief systemic and intraarticular (IA) half-lives of relaxin-2: 0.96 h and 0.62 h, respectively. Furthermore, using an established, immobilization murine model of shoulder arthrofibrosis, multiple IA injections of human relaxin-2 significantly improve ROM, returning it to baseline measurements collected before limb immobilization. This is in contrast to single IA (sIA) or multiple i.v. (mIV) injections of relaxin-2 with which the ROM remains constrained. The histological hallmarks of contracture (e.g., fibrotic adhesions and reduced joint space) are absent in the animals treated with multiple IA injections of relaxin-2 compared with the untreated control and the sIA-and mIV-treated animals. As these findings show, local delivery of relaxin-2 is an innovative treatment of shoulder arthrofibrosis. relaxin | fibrosis | frozen shoulder | arthrofibrosis

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Section: Significancementioning

confidence: 99%

Intraarticular injection of relaxin-2 alleviates shoulder arthrofibrosis

Blessing

Okajima

Cubria

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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“…Shown is the relative mean ± SEM dynamic lung compliance from control (saline), BLM-injured mice and from the various treatment groups investigated against BLM-induced pulmonary fibrosis, in response to the highest dose of methacholine evaluated (50 mg·ml −1 ). *P < 0.05, significantly different from the control group (SAL) ; # P < 0.05, significantly different from the BLM-treated group mast cells (Bani, Ballati, Masini, Bigazzi, & Sacchi, 1997), leukocytes (Bani et al, 1997;Pini, Boccalini, Lucarini, et al, 2016), and neutrophils (Masini et al, 2004) and suppressing the pro-inflammatory and profibrotic actions of TGF-β1 (Royce, Lim, et al, 2014;Unemori et al, 1996), TNF-α, IL-1β, and/or IL-18 (Brecht, Bartsch, Baumann, Stangl, & Dschietzig, 2011;Pini, Boccalini, Baccari, et al, 2016). Furthermore, serelaxin inhibits fibrosis by preventing fibroblast proliferation and differentiation into myofibroblasts as a means of limiting myofibroblastmediated ECM deposition Royce et al, 2015Royce et al, , 2016.…”

Section: Discussionmentioning

confidence: 95%

“…Combining exosomes with serelaxin could also have promoted synergistic actions through the activation of overlapping and distinct pathways. Serelaxin can inhibit the contribution of lung inflammation on fibrosis by reducing the infiltration and activation of mast cells (Bani, Ballati, Masini, Bigazzi, & Sacchi, ), leukocytes (Bani et al, ; Pini, Boccalini, Lucarini, et al, ), and neutrophils (Masini et al, ) and suppressing the pro‐inflammatory and pro‐fibrotic actions of TGF‐β1 (Royce, Lim, et al, ; Unemori et al, ), TNF‐α, IL‐1β, and/or IL‐18 (Brecht, Bartsch, Baumann, Stangl, & Dschietzig, ; Pini, Boccalini, Baccari, et al, ). Furthermore, serelaxin inhibits fibrosis by preventing fibroblast proliferation and differentiation into myofibroblasts as a means of limiting myofibroblast‐mediated ECM deposition (Huuskes et al, ; Royce et al, , ).…”

Section: Discussionmentioning

confidence: 99%

Serelaxin enhances the therapeutic effects of human amnion epithelial cell‐derived exosomes in experimental models of lung disease

Royce

Patel

Mao

et al. 2019

British J Pharmacology

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Background and Purpose There is growing interest in stem cell‐derived exosomes for their therapeutic and regenerative benefits given their manufacturing and regulatory advantages over cell‐based therapies. As existing fibrosis impedes the viability and efficacy of stem cell/exosome‐based strategies for treating chronic diseases, here we tested the effects of the anti‐fibrotic drug, serelaxin, on the therapeutic efficacy of human amnion epithelial cell (AEC)‐derived exosomes in experimental lung disease. Experimental Approach Female Balb/c mice were subjected to either the 9.5‐week model of ovalbumin and naphthalene (OVA/NA)‐induced chronic allergic airway disease (AAD) or 3‐week model of bleomycin (BLM)‐induced pulmonary fibrosis; then administered increasing concentrations of AEC‐exosomes (5 μg or 25μg), with or without serelaxin (0.5mg/kg/day) for 7‐days. 1x106 AECs co‐administered with serelaxin over the corresponding time‐period were included for comparison in both models, as was pirfenidone‐treatment of the BLM model. Control groups received saline/corn oil or saline, respectively. Key Results Both experimental models presented with significant tissue inflammation, remodelling, fibrosis and airway/lung dysfunction at the time‐points studied. While AEC‐exosome (5 μg or 25μg)‐administration alone demonstrated some benefits in each model, serelaxin was required for AEC‐exosomes (25μg) to rapidly normalise chronic AAD‐induced airway fibrosis and airway reactivity, and BLM‐induced lung inflammation, epithelial damage and subepithelial/basement membrane fibrosis. Combining serelaxin with AEC‐exosomes (25μg) also demonstrated broader protection compared to co‐administration of serelaxin with 1x106 AECs or pirfenidone. Conclusions and Implications Serelaxin enhanced the therapeutic efficacy of AEC‐exosomes in treating basement membrane‐induced fibrosis and related airway dysfunction.

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“…These studies in hypertensive models clearly show the vasculoprotective effects of relaxin against hypertension-induced dysfunction and its potential role in reversing hypertension-associated fibrosis. More recently, relaxin treatment is reported to reverse cigarette smoke-induced endothelial dysfunction, an effect attributed to enhanced endothelial NO synthase (eNOS) expression ( Pini et al, 2016 ). Relaxin infusion over 4 weeks also reverses the atherosclerosis-associated endothelial dysfunction in ApoE -/- mice, an effect attributed to reduction in angiotensin AT1 receptors and oxidative stress ( Tiyerili et al, 2016 ).…”

Section: Protective Role For Relaxin In the Vasculaturementioning

confidence: 99%

Relaxin as a Therapeutic Target for the Cardiovascular Complications of Diabetes

Leo

Parry

et al. 2018

Front. Pharmacol.

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Cardiovascular complications are the major cause of mortality in patients with diabetes. This is closely associated with both macrovascular and microvascular complications of diabetes, which lead to organ injuries in diabetic patients. Previous studies have consistently demonstrated the beneficial effects of relaxin treatment for protection of the vasculature, with evidence of antioxidant and anti-remodeling actions. Relaxin enhances nitric oxide, prostacyclin and endothelium-derived hyperpolarization (EDH)-type-mediated relaxation in various vascular beds. These effects of relaxin on the systemic vasculature, coupled with its cardiac actions, reduce pulmonary capillary wedge pressure and pulmonary artery pressure. This results in an overall decrease in systemic and pulmonary vascular resistance in heart failure patients. The anti-fibrotic actions of relaxin are well established, a desirable property in the context of diabetes. Further, relaxin ameliorates diabetic wound healing, with accelerated angiogenesis and vasculogenesis. Relaxin-mediated stimulation of vascular endothelial growth factor (VEGF) and stromal cell-derived factor 1-α, as well as regulation of metalloproteinase expression, ameliorates cardiovascular fibrosis in diabetic mice. In the heart, relaxin is a cardioprotective molecule in several experimental animal models, exerting anti-fibrotic, anti-hypertrophy and anti-apoptotic effects in diabetic pathologies. Collectively, these studies provide a foundation to propose the therapeutic potential for relaxin as an adjunctive agent in the prevention or treatment of diabetes-induced cardiovascular complications. This review provides a comprehensive overview of the beneficial effects of relaxin, and identifies its therapeutic possibilities for alleviating diabetes-related cardiovascular injury.

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

Cited by 34 publications

References 58 publications

Intraarticular injection of relaxin-2 alleviates shoulder arthrofibrosis

Intraarticular injection of relaxin-2 alleviates shoulder arthrofibrosis

Serelaxin enhances the therapeutic effects of human amnion epithelial cell‐derived exosomes in experimental models of lung disease

Relaxin as a Therapeutic Target for the Cardiovascular Complications of Diabetes

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