The Role of Mitochondrial Mutations in Chronification of Inflammation: Hypothesis and Overview of Own Data

The Role of Mitochondrial Mutations in Chronification of Inflammation: Hypothesis and Overview of Own Data

Chronic human diseases, especially age-related disorders, are often associated with chronic inflammation. It is currently not entirely clear what factors are responsible for the sterile inflammatory process becoming chronic in affected tissues. This process implies impairment of the normal resolutio...

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Bibliographic Details
Published in:Life (Basel, Switzerland) Vol. 12; no. 8; p. 1153
Main Authors: Orekhov, Alexander N., Nikiforov, Nikita G., Omelchenko, Andrey V., Sinyov, Vasily V., Sobenin, Igor A., Vinokurov, Andrey Y., Orekhova, Varvara A.
Format: Journal Article
Language:English
Published: Basel MDPI AG 29-07-2022
MDPI
Subjects:
Age
Age related diseases
Arteriosclerosis
Atherosclerosis
Bacteria
Cytokines
Cytology
Endothelium
Genomes
Hypotheses
Hypothesis
Immune system
Immunocompetence
Inflammation
Inflammatory response
Lesions
Mitochondria
Mitochondrial DNA
mitophagy
Mortality
mtDNA mutation
Mutagenesis
Mutation
Oxidative stress
Pathogenesis
Pathogens
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Summary:Chronic human diseases, especially age-related disorders, are often associated with chronic inflammation. It is currently not entirely clear what factors are responsible for the sterile inflammatory process becoming chronic in affected tissues. This process implies impairment of the normal resolution of the inflammatory response, when pro-inflammatory cytokine production ceases and tissue repair process begins. The important role of the mitochondria in the correct functioning of innate immune cells is currently well recognized, with mitochondrial signals being an important component of the inflammatory response regulation. In this work, we propose a hypothesis according to which mitochondrial DNA (mtDNA) mutations may play a key role in rendering certain cells prone to prolonged pro-inflammatory activation, therefore contributing to chronification of inflammation. The affected cells become sites of constant pro-inflammatory stimulation. The study of the distribution of atherosclerotic lesions on the surface of the arterial wall samples obtained from deceased patients revealed a focal distribution of lesions corresponding to the distribution of cells with altered morphology that are affected by mtDNA mutations. These observations support the proposed hypothesis and encourage further studies.
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ISSN:2075-1729
2075-1729
DOI:10.3390/life12081153