AI Article Synopsis
- Dysfunctions in mitochondrial fatty acid ß-oxidation (ß-FAO) are linked to common disorders like diabetes, obesity, and heart disease, showing its vital role in energy metabolism across key organs.
- Inborn defects in ß-FAO lead to a range of rare diseases, from severe conditions in newborns to adult-onset muscle issues, underlining its importance in high-energy-demand tissues.
- Recent studies suggest ß-FAO also influences non-energy functions, such as gene regulation and cellular behavior, indicating that targeting ß-FAO with drugs could be a new strategy for treating various diseases.
Article Abstract
Dysfunctions of mitochondrial fatty acid ß-oxidation (ß-FAO) in various tissues represent a hallmark of many common disorders, and are acknowledged to play an essential role in the pathogenesis of diabetes, obesity, and cardiac diseases. Moreover, inborn defects in ß-FAO form a large family of rare diseases with variable phenotypes, ranging from fatal multi-organ failure in the newborn to isolated adult onset myopathy. These pathologies highlight the critical role of ß-FAO in many tissues with high-energy demand (heart, muscle, liver, kidney). Furthermore, and unexpectedly, very recent data unveiled the possible involvement of ß-FAO in instructing complex non energy-related functions, such as chromatin modification, control of neural stem cell activity, or survival and fate of cancer cells. Pharmacological targeting of ß-FAO by small molecules might therefore open new avenues for the treatment of various rare or common diseases.
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| http://dx.doi.org/10.1051/medsci/2019156 | DOI Listing |
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