Proteomic and Mechanistic Analysis of Spironolactone in Patients at Risk for HF

João Pedro Ferreira; Job Verdonschot; Ping Wang; Anne Pizard; Timothy Collier; Fozia Z Ahmed; Hans-Peter Brunner-La-Rocca; Andrew L Clark; Franco Cosmi; Joe Cuthbert; Javier Díez; Frank Edelmann; Nicolas Girerd; Arantxa González; Stéphanie Grojean; Mark Hazebroek; Javed Khan; Roberto Latini; Mamas A Mamas; Beatrice Mariottoni; Blerim Mujaj; Pierpaolo Pellicori; Johannes Petutschnigg; Burkert Pieske; Patrick Rossignol; Philippe Rouet; Jan A Staessen; John G F Cleland; Stephane Heymans; Faiez Zannad; HOMAGE (Heart Omics in AGEing) Consortium

doi:10.1016/j.jchf.2020.11.010

Proteomic and Mechanistic Analysis of Spironolactone in Patients at Risk for HF

JACC Heart Fail. 2021 Apr;9(4):268-277. doi: 10.1016/j.jchf.2020.11.010. Epub 2021 Feb 3.

Authors

João Pedro Ferreira¹, Job Verdonschot², Ping Wang², Anne Pizard³, Timothy Collier⁴, Fozia Z Ahmed⁵, Hans-Peter Brunner-La-Rocca², Andrew L Clark⁶, Franco Cosmi⁷, Joe Cuthbert⁶, Javier Díez⁸, Frank Edelmann⁹, Nicolas Girerd¹⁰, Arantxa González⁸, Stéphanie Grojean³, Mark Hazebroek², Javed Khan¹⁰, Roberto Latini¹¹, Mamas A Mamas⁵, Beatrice Mariottoni⁷, Blerim Mujaj¹², Pierpaolo Pellicori¹⁰, Johannes Petutschnigg⁹, Burkert Pieske⁹, Patrick Rossignol³, Philippe Rouet¹³, Jan A Staessen¹², John G F Cleland¹⁰, Stephane Heymans², Faiez Zannad¹⁴; HOMAGE (Heart Omics in AGEing) Consortium

Affiliations

¹ Université de Lorraine, Inserm, Centre d'Investigation Clinique Plurithématique 1433, CHRU de Nancy, F-CRIN INI-CRCT, Nancy, France. Electronic address: j.ferreira@chru-nancy.fr.
² Department of Cardiology, Maastricht University Medical Center, the Netherlands.
³ Université de Lorraine, Inserm, Centre d'Investigation Clinique Plurithématique 1433, CHRU de Nancy, F-CRIN INI-CRCT, Nancy, France.
⁴ Department of Medical Statistics, London School of Hygiene and Tropical Medicine, London, United Kingdom.
⁵ Division of Cardiovascular Sciences, School of Medical Sciences, Faculty of Biology, Medicine and Health, Manchester Academic Health Science Centre, University of Manchester, Manchester, United Kingdom.
⁶ Department of Academic Cardiology, University of Hull, Castle Hill Hospital, Cottingham, United Kingdom.
⁷ Department of Cardiology, Cortona Hospital, Arezzo, Italy.
⁸ Program of Cardiovascular Diseases, CIMA Universidad de Navarra and IdiSNA, Pamplona, Spain; CIBERCV, Carlos III Institute of Health, Madrid, Spain.
⁹ Department of Internal Medicine/Cardiology, German Heart Center Berlin, Berlin, Germany.
¹⁰ Robertson Centre for Biostatistics, Institute of Health and Wellbeing, University of Glasgow, Glasgow Royal Infirmary, Glasgow, United Kingdom.
¹¹ Mario Negri Institute of Pharmacological Research-IRCCS, Milan, Italy.
¹² Studies Coordinating Centre, Research Unit Hypertension and Cardiovascular Epidemiology, Department of Cardiovascular Sciences, University of Leuven, Leuven, Belgium.
¹³ UMR UT3 CNRS 5288, Obesity and Heart Failure, Toulouse, France.
¹⁴ Université de Lorraine, Inserm, Centre d'Investigation Clinique Plurithématique 1433, CHRU de Nancy, F-CRIN INI-CRCT, Nancy, France. Electronic address: f.zannad@chru-nancy.fr.

PMID: 33549556
DOI: 10.1016/j.jchf.2020.11.010

Abstract

Objectives: This study sought to further understand the mechanisms underlying effect of spironolactone and assessed its impact on multiple plasma protein biomarkers and their respective underlying biologic pathways.

Background: In addition to their beneficial effects in established heart failure (HF), mineralocorticoid receptor antagonists may act upstream on mechanisms, preventing incident HF. In people at risk for developing HF, the HOMAGE (Heart OMics in AGEing) trial showed that spironolactone treatment could provide antifibrotic and antiremodeling effects, potentially slowing the progression to HF.

Methods: Baseline, 1-month, and 9-month (or last visit) plasma samples of HOMAGE participants were measured for protein biomarkers (n = 276) by using Olink Proseek-Multiplex cardiovascular and inflammation panels (Olink, Uppsala, Sweden). The effect of spironolactone on biomarkers was assessed by analysis of covariance and explored by knowledge-based network analysis.

Results: A total of 527 participants were enrolled; 265 were randomized to spironolactone (25 to 50 mg/day) and 262 to standard care ("control"). The median (interquartile range) age was 73 years (69 to 79 years), and 26% were female. Spironolactone reduced biomarkers of collagen metabolism (e.g., COL1A1, MMP-2); brain natriuretic peptide; and biomarkers related to metabolic processes (e.g., PAPPA), inflammation, and thrombosis (e.g., IL17A, VEGF, and urokinase). Spironolactone increased biomarkers that reflect the blockade of the mineralocorticoid receptor (e.g., renin) and increased the levels of adipokines involved in the anti-inflammatory response (e.g., RARRES2) and biomarkers of hemostasis maintenance (e.g., tPA, UPAR), myelosuppressive activity (e.g., CCL16), insulin suppression (e.g., RETN), and inflammatory regulation (e.g., IL-12B).

Conclusions: Proteomic analyses suggest that spironolactone exerts pleiotropic effects including reduction in fibrosis, inflammation, thrombosis, congestion, and vascular function improvement, all of which may mediate cardiovascular protective effects, potentially slowing progression toward heart failure. (HOMAGE [Bioprofiling Response to Mineralocorticoid Receptor Antagonists for the Prevention of Heart Failure]; NCT02556450).

Keywords: fibrosis; heart failure prevention; inflammation; renin-angiotensin-aldosterone system; spironolactone.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Aged
Female
Heart Failure* / drug therapy
Humans
Male
Mineralocorticoid Receptor Antagonists / therapeutic use
Natriuretic Peptide, Brain
Proteomics
Spironolactone* / therapeutic use

Substances

Mineralocorticoid Receptor Antagonists
Natriuretic Peptide, Brain
Spironolactone

Associated data

ClinicalTrials.gov/NCT02556450