Mitochondria‐derived damage‐associated molecular patterns and inflammation in the ischemic‐reperfused heart

Author:

Torp May‐Kristin1ORCID,Vaage Jarle123,Stensløkken Kåre‐Olav1

Affiliation:

1. Division of Physiology, Department of Molecular Medicine Institute of Basic Medical Sciences, University of Oslo Oslo Norway

2. Institute of Clinical Medicine University of Oslo Oslo Norway

3. Department of Research and Development, Division of Emergencies and Critical Care Oslo University Hospital Oslo Norway

Abstract

AbstractCardiac cell death after myocardial infarction release endogenous structures termed damage‐associated molecular patterns (DAMPs) that trigger the innate immune system and initiate a sterile inflammation in the myocardium. Cardiomyocytes are energy demanding cells and 30% of their volume are mitochondria. Mitochondria are evolutionary endosymbionts originating from bacteria containing molecular patterns similar to bacteria, termed mitochondrial DAMPs (mDAMPs). Consequently, mitochondrial debris may be particularly immunogenic and damaging. However, the role of mDAMPs in myocardial infarction is not clarified. Identifying the most harmful mDAMPs and inhibiting their early inflammatory signaling may reduce infarct size and the risk of developing post‐infarct heart failure. The focus of this review is the role of mDAMPs in the immediate pro‐inflammatory phase after myocardial infarction before arrival of immune cells in the myocardium. We discuss different mDAMPs, their role in physiology and present knowledge regarding their role in the inflammatory response of acute myocardial infarction.

Funder

Universitetet i Oslo

Publisher

Wiley

Subject

Physiology

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