Risk Assessment of Psychotropic Drugs on Mitochondrial Function Using In Vitro Assays.

Biomedicines

Department of Pharmaceutical Sciences, Barry & Judy Silverman College of Pharmacy, Nova Southeastern University, 3200 South University Drive, Ft. Lauderdale, FL 33328-2018, USA.

Published: December 2023

AI Article Synopsis

  • This study explores how 22 psychotropic drugs affect mitochondrial function, specifically looking at their potential to cause organ toxicity.
  • Several drugs were found to inhibit the electron transport chain (ETC) or act as uncouplers, with varying levels of cytotoxicity identified in HepG2 cells and isolated rat liver mitochondria.
  • The findings help clarify the molecular mechanisms behind drug-induced mitochondrial toxicity, which can inform safer clinical drug choices.

Article Abstract

Mitochondria are potential targets responsible for some drug- and xenobiotic-induced organ toxicities. However, molecular mechanisms of drug-induced mitochondrial toxicities are mostly unknown. Here, multiple in vitro assays were used to investigate the effects of 22 psychotropic drugs on mitochondrial function. The acute extracellular flux assay identified inhibitors of the electron transport chain (ETC), i.e., aripiprazole, phenytoin, and fluoxetine, an uncoupler (reserpine), substrate inhibitors (quetiapine, carbamazepine, buspirone, and tianeptine), and cytotoxic compounds (chlorpromazine and valproic acid) in HepG2 cells. Using permeabilized HepG2 cells revealed minimum effective concentrations of 66.3, 6730, 44.5, and 72.1 µM for the inhibition of complex-I-linked respiration for quetiapine, valproic acid, buspirone, and fluoxetine, respectively. Assessing complex-II-linked respiration in isolated rat liver mitochondria revealed haloperidol is an ETC inhibitor, chlorpromazine is an uncoupler in basal respiration and an ETC inhibitor under uncoupled respiration (IC = 135 µM), while olanzapine causes a mild dissipation of the membrane potential at 50 µM. This research elucidates some mechanisms of drug toxicity and provides some insight into their safety profile for clinical drug decisions.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10741027PMC
http://dx.doi.org/10.3390/biomedicines11123272DOI Listing

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