AI Article Synopsis

  • Mitochondrial dysfunction is linked to various psychiatric and neurologic diseases, stemming from factors like DNA mutations, impaired antioxidant defenses, hormonal issues, and metabolic problems.
  • The main effects of mitochondrial dysfunction are increased oxidative stress and energy crises in cells.
  • Current antioxidant therapies haven't been universally effective due to the complexity of mitochondrial issues, prompting a proposed new antioxidant strategy aimed at alleviating oxidative stress and enhancing energy production in affected patients.

Article Abstract

Mitochondrial dysfunction is at the base of development and progression of several psychiatric and neurologic diseases with different etiologies. MtDNA/nDNA mutational damage, failure of endogenous antioxidant defenses, hormonal malfunction, altered membrane permeability, metabolic dysregulation, disruption of calcium buffering capacity and ageing have been found to be the root causes of mitochondrial dysfunction in psychatric and neurodegenerative diseases. However, the overall consequences of mitochondrial dysfunction are only limited to increase in oxidative/nitrosative stress and cellular energy crises. Thus far, extensive efforts have been made to improve mitochondrial function through specific cause-dependent antioxidant therapy. However, owing to complex genetic and interlinked causes of mitochondrial dysfunction, it has not been possible to achieve any common, unique supportive antioxidant therapeutic strategy for the treatment of psychiatric and neurologic diseases. Hence, we propose an antioxidant therapeutic strategy for management of consequences of mitochondrial dysfunction in psychiatric and neurologic diseases. It is expected that this will not only reduces oxidative stress, but also promote anaerobic energy production.

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Source
http://dx.doi.org/10.1002/biof.1093DOI Listing

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