Mitochondrion

Mitochondria are organelles found in all cells that have a nucleus. In the human body, that would be all cells except red blood cells. They generate most of a cell's energy by manufacturing adenosine triphosphate, ATP. Mitochondria have their own independent genome called mitochondrial DNA.

Biogenesis
Mitochondrial biogenesis (the creation of new mitochondria) can be increased via hormesis, the exposure of the body to short-term stressors. Healthy stressors include exercise, fasting, cold, heat and light. Resveratrol can also increase mitochondrial biogenesis.

Infection and immunity
Mitochondria play crucial role in innate immunity, namely through their induction of interferon production and apoptosis through mitochondrial antiviral signaling protein (MAVS). Many viruses, including Coxsackievirus B3, echovirus 7 and enterovirus 71, inhibit interferon induction and evade host immunity by cleaving or downregulating MAVS.

Herpes simplex virus (HSV-1), influenza, and poliovirus have all been found to reduce cellular respiration. Hepatitis C reduces aerobic metabolism and upregulates glycolysis.

In human disease
Infection with pathogens, including viruses, bacteria, and parasites, can all induce changes in mitochondrial function and energy metabolism.

Viruses can induce or inhibit mitochondrial processes in order to replicate. "Viruses like Herpes simplex virus 1 deplete the host mitochondrial DNA and some, like human immunodeficiency virus and Hepatitis C Virus, hijack the host mitochondrial proteins to function fully inside the host cell." Hepatitis C has also been shown to "fragment host mitochondria".

Parasites such as Toxoplasma gondii have also been shown to modulate host energy metabolism and dysregulate mitochondrial function,, as have bacteria such as E. coli, which has been shown to modulate mitochondrial receptor function.

Mitochondrial disease has a high prevalence of fatigue and debilitation.

Chronic fatigue syndrome
There is evidence of mitochondrial dysfunction in chronic fatigue syndrome patients. Muscle biopsies have shown evidence of mitochondrial degeneration, deletions of mitochondrial DNA , the reduction of mitochondrial activity , and Sarah Myhill found measurable mitochondrial dysfunction correlating with severity of illness. Myhill also produced improvement by targeting those dysfunctions. Mitochondrial DNA variants correlate with symptoms, symptom clusters & symptom severity.

Mitochondrial disorders can be mistaken for chronic fatigue syndrome.

There is evidence of genetic risk factors for mitochondrial dysfunction in related diseases such as complex regional pain syndrome, postural orthostatic tachycardia syndrome (POTS), and dysautonomia.

Notable studies

 * 1997, Chronic fatigue syndrome and skeletal muscle mitochondrial function
 * 2015, Metabolic profiling reveals anomalous energy metabolism and oxidative stress pathways in chronic fatigue syndrome patients


 * 2016, Exercise-induced mitochondrial dysfunction: a myth or reality?
 * 2016, Pharmacological NAD-Boosting Strategies Improve Mitochondrial Homeostasis in Human Complex I-Mutant Fibroblasts
 * 2018, Parkin and PINK1 mitigate STING-induced inflammation

Videos

 * "Mitochondria: The Powerhouse of the Cell" by Bozeman Science

Learn more

 * CFS - The Central Cause - Mitochondrial Failure


 * Wikipedia - Mitochondrion
 * 2016, Immune System Conserves Energy By Altering Metabolism
 * 2016, ME Association to fund fourth study into the role of the mitochondria in ME/CFS
 * 2016, ME Association Goes All in on the Mitochondria in Chronic Fatigue Syndrome (ME/CFS)
 * 2016, Australian metabolomics study of young women with ME/CFS (CCC)
 * 2016, "Mitochondria Man Gets Money UK Goes Mega Chronic Fatigue Syndrome Research Moves Forward"

Unused Citations
Armstrong2014 Craig2015 Vermeulen2010 Maes2009 Morris2013. Morris2014 Meeus2013

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