Circulating Gal‐3 and sST2 are associated with acute exercise‐induced sustained endothelial activation: Possible relevance for fibrosis development?

Julia M. Kröpfl; Fernando G. Beltrami; Hans‐Jürgen Gruber; Arno Schmidt‐Trucksäss; Thomas Dieterle; Christina M. Spengler

doi:10.1113/EP091277

Experimental Physiology (Oct 2023)

Circulating Gal‐3 and sST2 are associated with acute exercise‐induced sustained endothelial activation: Possible relevance for fibrosis development?

Julia M. Kröpfl,
Fernando G. Beltrami,
Hans‐Jürgen Gruber,
Arno Schmidt‐Trucksäss,
Thomas Dieterle,
Christina M. Spengler

Affiliations

Julia M. Kröpfl: Division of Sport and Exercise Medicine, Department of Sport, Exercise and Health University of Basel Basel Switzerland
Fernando G. Beltrami: Exercise Physiology Lab, Institute of Human Movement Sciences and Sport ETH Zurich Zurich Switzerland
Hans‐Jürgen Gruber: Clinical Institute of Medical and Chemical Laboratory Diagnostics Medical University of Graz Graz Austria
Arno Schmidt‐Trucksäss: Division of Sport and Exercise Medicine, Department of Sport, Exercise and Health University of Basel Basel Switzerland
Thomas Dieterle: Foeldiklinik GmbH&Co KG Hinterzarten Germany
Christina M. Spengler: Exercise Physiology Lab, Institute of Human Movement Sciences and Sport ETH Zurich Zurich Switzerland

DOI: https://doi.org/10.1113/EP091277
Journal volume & issue: Vol. 108, no. 10
pp. 1259 – 1267

Abstract

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Abstract Long‐term, intense endurance exercise training can occasionally induce endothelial micro‐damage and cardiac fibrosis. The underlying mechanisms are incompletely understood. Twenty healthy, well‐trained male participants (10 runners and 10 cyclists) performed a strenuous high‐intensity interval training (HIIT) session matched by age, height, weight and maximal oxygen consumption. We assessed the acute exercise response of novel cardiac biomarkers of fibrosis [e.g., galectin‐3 (Gal‐3) and soluble suppression of tumorigenicity 2 (sST2)] per exercise modality and their relationship with haemodynamic contributors, such as preload, afterload and cardiac contractility index (CTi), in addition to endothelial damage by sustained activation and shedding of endothelial cells (ECs). Serum Gal‐3 and sST2 concentrations were investigated by enzyme‐linked immunosorbent assays; haemodynamics were analysed via impedance plethysmography and circulating ECs by flow cytometry. The Gal‐3 and sST2 concentrations and ECs were elevated after exercise (P < 0.001), without interaction between exercise modalities. Circulating Gal‐3 and sST2 concentrations both showed a positive relationship with ECs (rrm = 0.68, P = 0.001 and rrm = 0.57, P = 0.010, respectively, both n = 18). The EC association with Gal‐3 was significant only in cyclists, but equally strong for both modalities. Gal‐3 was also related to exercise‐induced CTi (rrm = 0.57, P = 0.011, n = 18). Cardiac wall stress is increased after an acute HIIT session but does not differ between exercise modalities. Exercise‐released Gal‐3 from cardiac macrophages could very probably drive systemic endothelial damage, based on an enhanced CTi. The importance of acute exercise‐induced vascular resistances and cardiac contractility for the release of fibrotic biomarkers and any long‐term pathological endothelial adaptation should be investigated further, also relative to the exercise modality.

Published in Experimental Physiology

ISSN: 0958-0670 (Print); 1469-445X (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Physiology
Website: https://physoc.onlinelibrary.wiley.com/journal/1469445X

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