Cells (Mar 2022)

Mitochondrial Respiratory Complexes as Targets of Drugs: The PPAR Agonist Example

  • Patrizia Bottoni,
  • Alessandro Pontoglio,
  • Salvatore Scarà,
  • Luisa Pieroni,
  • Andrea Urbani,
  • Roberto Scatena

DOI
https://doi.org/10.3390/cells11071169
Journal volume & issue
Vol. 11, no. 7
p. 1169

Abstract

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Mitochondrial bioenergetics are progressively acquiring significant pathophysiological roles. Specifically, mitochondria in general and Electron Respiratory Chain in particular are gaining importance as unintentional targets of different drugs. The so-called PPAR ligands are a class of drugs which not only link and activate Peroxisome Proliferator-Activated Receptors but also show a myriad of extrareceptorial activities as well. In particular, they were shown to inhibit NADH coenzyme Q reductase. However, the molecular picture of this intriguing bioenergetic derangement has not yet been well defined. Using high resolution respirometry, both in permeabilized and intact HepG2 cells, and a proteomic approach, the mitochondrial bioenergetic damage induced by various PPAR ligands was evaluated. Results show a derangement of mitochondrial oxidative metabolism more complex than one related to a simple perturbation of complex I. In fact, a partial inhibition of mitochondrial NADH oxidation seems to be associated not only with hampered ATP synthesis but also with a significant reduction in respiratory control ratio, spare respiratory capacity, coupling efficiency and, last but not least, serious oxidative stress and structural damage to mitochondria.

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