Literature DB >> 27418970

Serelaxin for the treatment of acute heart failure: a review with a focus on end-organ protection.

Javier Díez1, Luis M Ruilope2.   

Abstract

Acute heart failure (AHF) is a complex clinical syndrome characterized by fluid overload and haemodynamic abnormalities (short-term clinical consequences) and the development of end-organ damage (long-term consequences). Current therapies for the treatment of AHF, such as loop diuretics and vasodilators, help to relieve haemodynamic imbalance and congestion, but have not been shown to prevent (and may even contribute to) end-organ damage, or to provide long-term clinical benefit. Serelaxin is the recombinant form of human relaxin-2, a naturally occurring hormone involved in mediating haemodynamic changes during pregnancy. Preclinical and clinical studies have investigated the effects mediated by serelaxin and the suitability of this agent for the treatment of patients with AHF. Data suggest that serelaxin acts via multiple pathways to improve haemodynamics at the vascular, cardiac, and renal level and provide effective congestion relief. In addition, this novel agent may protect the heart, kidneys, and liver from damage by inhibiting inflammation, oxidative stress, cell death, and tissue fibrosis, and stimulating angiogenesis. Serelaxin may therefore improve both short- and long-term outcomes in patients with AHF. In this review, we examine the unique mechanisms underlying the potential benefits of serelaxin for the treatment of AHF, in particular, those involved in mediating end-organ protection.
© The Author 2015. Published by Oxford University Press on behalf of the European Society of Cardiology.

Entities:  

Keywords:  Acute heart failure; Congestion relief; Long-term outcomes; Organ protection; Serelaxin

Mesh:

Substances:

Year:  2015        PMID: 27418970      PMCID: PMC4853824          DOI: 10.1093/ehjcvp/pvv046

Source DB:  PubMed          Journal:  Eur Heart J Cardiovasc Pharmacother


  127 in total

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Journal:  J Am Coll Cardiol       Date:  2010-09-28       Impact factor: 24.094

2.  Relaxin counteracts myocardial damage induced by ischemia-reperfusion in isolated guinea pig hearts: evidence for an involvement of nitric oxide.

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Authors:  Edna D Lekgabe; Helen Kiriazis; Chongxin Zhao; Qi Xu; Xiao Lei Moore; Yidan Su; Ross A D Bathgate; Xiao-Jun Du; Chrishan S Samuel
Journal:  Hypertension       Date:  2005-06-20       Impact factor: 10.190

4.  Relaxin as a protective substance in the preserving solution for liver transplantation: spectrophotometric in vivo imaging of local oxygen supply in an isolated perfused rat liver model.

Authors:  Markus U Boehnert; Franz Paul Armbruster; Heidegard Hilbig
Journal:  Ann N Y Acad Sci       Date:  2009-04       Impact factor: 5.691

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Journal:  Am J Pathol       Date:  1998-05       Impact factor: 4.307

Review 6.  Nitrate therapy: new aspects concerning molecular action and tolerance.

Authors:  Thomas Münzel; Andreas Daiber; Tommaso Gori
Journal:  Circulation       Date:  2011-05-17       Impact factor: 29.690

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Authors:  L L Konecke
Journal:  J Clin Pharmacol       Date:  1981 Nov-Dec       Impact factor: 3.126

8.  Relaxin-induced reduction of infarct size in male rats receiving MCAO is dependent on nitric oxide synthesis and not estrogenic mechanisms.

Authors:  Brian C Wilson; Barry Connell; Tarek M Saleh
Journal:  Neurosci Lett       Date:  2005-10-17       Impact factor: 3.046

9.  Relaxin signals through a RXFP1-pERK-nNOS-NO-cGMP-dependent pathway to up-regulate matrix metalloproteinases: the additional involvement of iNOS.

Authors:  Bryna Suet Man Chow; Elaine Guo Yan Chew; Chongxin Zhao; Ross A D Bathgate; Tim D Hewitson; Chrishan S Samuel
Journal:  PLoS One       Date:  2012-08-22       Impact factor: 3.240

10.  Acute intravenous injection of serelaxin (recombinant human relaxin-2) causes rapid and sustained bradykinin-mediated vasorelaxation.

Authors:  Chen Huei Leo; Maria Jelinic; Helena C Parkington; Marianne Tare; Laura J Parry
Journal:  J Am Heart Assoc       Date:  2014-02-28       Impact factor: 5.501

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  6 in total

Review 1.  Pharmacologic Management for Heart Failure and Emerging Therapies.

Authors:  Diana H Kim; Feng-Ju Chien; Howard J Eisen
Journal:  Curr Cardiol Rep       Date:  2017-08-24       Impact factor: 2.931

2.  Morphine in acute heart failure.

Authors:  Stefan Agewall
Journal:  J Thorac Dis       Date:  2017-07       Impact factor: 2.895

3.  Relaxin Family Member Insulin-Like Peptide 6 Ameliorates Cardiac Fibrosis and Prevents Cardiac Remodeling in Murine Heart Failure Models.

Authors:  Sonomi Maruyama; Chia-Ling Wu; Sumiko Yoshida; Dongying Zhang; Pei-Hsuan Li; Fangzhou Wu; Jennifer Parker Duffen; Rouan Yao; Blake Jardin; Ibrahim M Adham; Ronald Law; Joel Berger; Richard Di Marchi; Kenneth Walsh
Journal:  J Am Heart Assoc       Date:  2018-06-10       Impact factor: 5.501

4.  Rationale and design of the AUGUST-AHF Study.

Authors:  Jingjing Zhang; Yang Sun; Kehua Zhou; Xiaoyu Zhang; Ying Chen; Jiayuan Hu; Changming Zhong; Yan Liu; Hongcai Shang
Journal:  ESC Heart Fail       Date:  2020-06-22

Review 5.  Relaxin-2 as a Potential Biomarker in Cardiovascular Diseases.

Authors:  Alana Aragón-Herrera; Sandra Feijóo-Bandín; Laura Anido-Varela; Sandra Moraña-Fernández; Esther Roselló-Lletí; Manuel Portolés; Estefanía Tarazón; Oreste Gualillo; José Ramón González-Juanatey; Francisca Lago
Journal:  J Pers Med       Date:  2022-06-21

6.  Serelaxin improves cardiac and renal function in DOCA-salt hypertensive rats.

Authors:  Dong Wang; Yuhuan Luo; Komuraiah Myakala; David J Orlicky; Evgenia Dobrinskikh; Xiaoxin Wang; Moshe Levi
Journal:  Sci Rep       Date:  2017-08-29       Impact factor: 4.379

  6 in total

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