The landmark year 1988 can be considered as the birthdate of mitochondrial medicine, when the first pathogenic mutations affecting mtDNA were associated with human diseases. Three decades later, the field still expands and we are not ‘scraping the bottom of the barrel’ yet. Despite the tremendous progress in terms of molecular characterization and genotype/phenotype correlations, for the vast majority of cases we still lack a deep understanding of the pathogenesis, good models to study, and effective therapeutic options. However, recent technological advances including somatic cell reprogramming to induced pluripotent stem cells (iPSCs), organoid technology, and tailored endonucleases provide unprecedented opportunities to fill these gaps, casting hope to soon cure the major primary mitochondrial phenotypes reviewed here. This group of rare diseases represents a key model for tackling the pathogenic mechanisms involving mitochondrial biology relevant to much more common disorders that affect our currently ageing population, such as diabetes and metabolic syndrome, neurodegenerative and inflammatory disorders, and cancer.

Keywords:
Chronic Progressive External Ophthalmoplegia, MELAS, MERRF, LHON, mitochondrial DNA mutations, Kearn-Sayre Syndrome
Subjects:
Diabetes & Metabolic Disorders, Molecular Bases of Health & Disease, Organelles & Localization, Pharmacology & Toxicology
© 2018 The Author(s). Published by Portland Press Limited on behalf of the Biochemical Society
2018
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