Mitochondrial dysfunction and damage associated molecular patterns (DAMPs) in chronic inflammatory diseases

Cruz, Charles S. Dela; Kang, Min

doi:10.1016/j.mito.2017.12.001

Cited by 149 publications

(65 citation statements)

References 106 publications

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“…Mitochondrial DAMPs retain at least two unique molecular features that are evolutionary endosymbionts derived from bacteria: mtDNA rich in unmethylated CpG motifs and N-formyl peptides. Emerging evidence suggests that mtDNA and N-formyl peptides act on TLR9 and formyl peptide receptors, respectively, to induce inflammatory responses through the assembly of the NLRP3 inflammasome (143)(144)(145)(146).…”

Section: Mitochondrial Dysfunction and Inflammation In Heart Failurementioning

confidence: 99%

Mitochondrial dysfunction in pathophysiology of heart failure

Zhou¹,

Tian²

2018

Journal of Clinical Investigation

542

485

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Mitochondrial dysfunction has been implicated in the development of heart failure. Oxidative metabolism in mitochondria is the main energy source of the heart, and the inability to generate and transfer energy has long been considered the primary mechanism linking mitochondrial dysfunction and contractile failure. However, the role of mitochondria in heart failure is now increasingly recognized to be beyond that of a failed power plant. In this Review, we summarize recent evidence demonstrating vicious cycles of pathophysiological mechanisms during the pathological remodeling of the heart that drive mitochondrial contributions from being compensatory to being a suicide mission. These mechanisms include bottlenecks of metabolic flux, redox imbalance, protein modification, ROS-induced ROS generation, impaired mitochondrial Ca2+ homeostasis, and inflammation. The interpretation of these findings will lead us to novel avenues for disease mechanisms and therapy.

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Section: Mitochondrial Dysfunction and Inflammation In Heart Failurementioning

confidence: 99%

Mitochondrial dysfunction in pathophysiology of heart failure

Zhou¹,

Tian²

2018

Journal of Clinical Investigation

542

485

View full text Add to dashboard Cite

show abstract

“…In that context, the mitochondria, derived several billions of years ago from the endosymbiosis of α-proteobacteria into a eukaryotic cell, represent a smorgasbord of potential immune-stimulating DAMPs. Putative mitochondrial DAMPs include the release of mitochondrial DNA (mtDNA), N-formyl peptides generated by translation of mitochondrial-encoded protein, and unique lipid species such as cardiolipin, a unique phospholipid enriched on the inner mitochondrial membrane (25). In the case of circulating mtDNA, immune activation occurs, in part, by activation of Toll-like receptor 9 (TLR9) signaling, while for mitochondrial proteins, activation occurs through binding to formyl peptide receptor-1.…”

Section: Mitochondria and The Inflammation Of Agingmentioning

confidence: 99%

The role of mitochondria in aging

Jang

Blum

Liu

et al. 2018

Journal of Clinical Investigation

292

241

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The biological basis of human aging remains one of the greatest unanswered scientific questions. Increasing evidence, however, points to a role for alterations in mitochondrial function as a potential central regulator of the aging process. Here, we focus primarily on three aspects of mitochondrial biology that link this ancient organelle to how and why we age. In particular, we discuss the role of mitochondria in regulating the innate immune system, the mechanisms linking mitochondrial quality control to age-dependent pathology, and the possibility that mitochondrial-to-nuclear signaling might regulate the rate of aging.

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“…It is currently clear that mitochondrial dysfunction and damage is involved in NLRP3 inflammasomes activation [60]. Dysfunctional mitochondria serve as an important source of DAMPs and as the inducers of cells oxidative damage and death implicated in several chronic human pathologies [63].…”

Section: Innate Immunity Response and Cellular Mechanisms Of Inflammamentioning

confidence: 99%

Possible Role of Mitochondrial DNA Mutations in Chronification of Inflammation: Focus on Atherosclerosis

Orekhov

Nikiforov

Ivanova

et al. 2020

JCM

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Chronification of inflammation is the process that lies at the basis of several human diseases that make up to 80% of morbidity and mortality worldwide. It can also explain a great deal of processes related to aging. Atherosclerosis is an example of the most important chronic inflammatory pathology in terms of public health impact. Atherogenesis is based on the inflammatory response of the innate immunity arising locally or focally. The main trigger for this response appears to be modified low-density lipoprotein (LDL), although other factors may also play a role. With the quick resolution of inflammation, atherosclerotic changes in the arterial wall do not occur. However, a violation of the innate immunity response can lead to chronification of local inflammation and, as a result, to atherosclerotic lesion formation. In this review, we discuss possible mechanisms of the impaired immune response with a special focus on mitochondrial dysfunction. Some mitochondrial dysfunctions may be due to mutations in mitochondrial DNA. Several mitochondrial DNA mutations leading to defective mitophagy have been identified. The regulatory role of mitophagy in the immune response has been shown in recent studies. We suggest that defective mitophagy promoted by mutations in mitochondrial DNA can cause innate immunity disorders leading to chronification of inflammation.

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Mitochondrial dysfunction and damage associated molecular patterns (DAMPs) in chronic inflammatory diseases

Cited by 149 publications

References 106 publications

Mitochondrial dysfunction in pathophysiology of heart failure

Mitochondrial dysfunction in pathophysiology of heart failure

The role of mitochondria in aging

Possible Role of Mitochondrial DNA Mutations in Chronification of Inflammation: Focus on Atherosclerosis

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