Enhanced cardiac hypoxic injury in atherogenic dyslipidaemia results from alterations in the energy metabolism pattern

Mariola Olkowicz; Marta Tomczyk; Janusz Debski; Urszula Tyrankiewicz; Kamil Przyborowski; Tomasz Borkowski; Magdalena Zabielska-Kaczorowska; Natalia Szupryczynska; Zdzislaw Kochan; Marta Smeda; Michal Dadlez; Stefan Chlopicki; Ryszard T Smolenski

doi:10.1016/j.metabol.2020.154400

Enhanced cardiac hypoxic injury in atherogenic dyslipidaemia results from alterations in the energy metabolism pattern

Metabolism. 2021 Jan:114:154400. doi: 10.1016/j.metabol.2020.154400. Epub 2020 Oct 13.

Affiliations

¹ Department of Biochemistry, Faculty of Medicine, Medical University of Gdansk, 1 Debinki St., 80-211 Gdansk, Poland; Jagiellonian Centre for Experimental Therapeutics (JCET), Jagiellonian University, 14 Bobrzynskiego St., 30-348 Krakow, Poland.
² Department of Biochemistry, Faculty of Medicine, Medical University of Gdansk, 1 Debinki St., 80-211 Gdansk, Poland.
³ Mass Spectrometry Laboratory, Institute of Biochemistry and Biophysics, Polish Academy of Sciences, 5a Pawinskiego St., 02-106 Warsaw, Poland.
⁴ Jagiellonian Centre for Experimental Therapeutics (JCET), Jagiellonian University, 14 Bobrzynskiego St., 30-348 Krakow, Poland.
⁵ Department of Biochemistry, Faculty of Medicine, Medical University of Gdansk, 1 Debinki St., 80-211 Gdansk, Poland; Department of Physiology, Faculty of Medicine, Medical University of Gdansk, 1 Debinki St., 80-211 Gdansk, Poland.
⁶ Department of Nutritional Biochemistry, Faculty of Health Sciences, Medical University of Gdansk, 7 Debinki St., 80-211 Gdansk, Poland.
⁷ Jagiellonian Centre for Experimental Therapeutics (JCET), Jagiellonian University, 14 Bobrzynskiego St., 30-348 Krakow, Poland; Chair of Pharmacology, Jagiellonian University Medical College, 16 Grzegorzecka St., 31-531 Krakow, Poland. Electronic address: stefan.chlopicki@jcet.eu.
⁸ Department of Biochemistry, Faculty of Medicine, Medical University of Gdansk, 1 Debinki St., 80-211 Gdansk, Poland. Electronic address: rt.smolenski@gumed.edu.pl.

PMID: 33058853
DOI: 10.1016/j.metabol.2020.154400

Abstract

Objective: Dyslipidaemia is a major risk factor for myocardial infarction that is known to correlate with atherosclerosis in the coronary arteries. We sought to clarify whether metabolic alterations induced by dyslipidaemia in cardiomyocytes collectively constitute an alternative pathway that escalates myocardial injury.

Methods: Dyslipidaemic apolipoprotein E and low-density lipoprotein receptor (ApoE/LDLR) double knockout (ApoE^-/-/LDLR^-/-) and wild-type C57BL/6 (WT) mice aged six months old were studied. Cardiac injury under reduced oxygen supply was evaluated by 5 min exposure to 5% oxygen in the breathing air under electrocardiogram (ECG) recording and with the assessment of troponin I release. To address the mechanisms LC/MS was used to analyse the cardiac proteome pattern or in vivo metabolism of stable isotope-labelled substrates and HPLC was applied to measure concentrations of cardiac high-energy phosphates. Furthermore, the effect of blocking fatty acid use with ranolazine on the substrate preference and cardiac hypoxic damage was studied in ApoE^-/-/LDLR^-/- mice.

Results: Hypoxia induced profound changes in ECG ST-segment and troponin I leakage in ApoE^-/-/LDLR^-/- mice but not in WT mice. The evaluation of the cardiac proteomic pattern revealed that ApoE^-/-/LDLR^-/- as compared with WT mice were characterised by coordinated increased expression of mitochondrial proteins, including enzymes of fatty acids' and branched-chain amino acids' oxidation, accompanied by decreased expression levels of glycolytic enzymes. These findings correlated with in vivo analysis, revealing a reduction in the entry of glucose and enhanced entry of leucine into the cardiac Krebs cycle, with the cardiac high-energy phosphates pool maintained. These changes were accompanied by the activation of molecular targets controlling mitochondrial metabolism. Ranolazine reversed the oxidative metabolic shift in ApoE^-/-/LDLR^-/- mice and reduced cardiac damage induced by hypoxia.

Conclusions: We suggest a novel mechanism for myocardial injury in dyslipidaemia that is consequent to an increased reliance on oxidative metabolism in the heart. The alterations in the metabolic pattern that we identified constitute an adaptive mechanism that facilitates maintenance of metabolic equilibrium and cardiac function under normoxia. However, this adaptation could account for myocardial injury even in a mild reduction of oxygen supply.

Keywords: Atherosclerotic mice; Dyslipidaemia; Mitochondria; Myocardial injury; Myocardial metabolic remodelling.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apolipoproteins E / genetics
Apolipoproteins E / metabolism
Atherosclerosis / metabolism*
Coronary Artery Disease / metabolism
Dyslipidemias / metabolism*
Electrocardiography
Energy Metabolism / physiology*
Mice
Mice, Knockout
Myocardial Infarction / metabolism*
Myocytes, Cardiac / metabolism*
Receptors, LDL / genetics
Receptors, LDL / metabolism
Troponin I / metabolism

Substances

Apolipoproteins E
Receptors, LDL
Troponin I