TY - JOUR
T1 - Real-time monitoring of oxygen uptake in hepatic bioreactor shows CYP450-independent mitochondrial toxicity of acetaminophen and amiodarone
AU - Prill, Sebastian
AU - Bavli, Danny
AU - Levy, Gahl
AU - Ezra, Elishai
AU - Schmälzlin, Elmar
AU - Jaeger, Magnus S
AU - Schwarz, Michael
AU - Duschl, Claus
AU - Cohen, Merav
AU - Nahmias, Yaakov
N1 - Publisher Copyright:
© 2015, Springer-Verlag Berlin Heidelberg.
PY - 2016/5
Y1 - 2016/5
N2 - Prediction of drug-induced toxicity is complicated by the failure of animal models to extrapolate human response, especially during assessment of repeated dose toxicity for cosmetic or chronic drug treatments. In this work, we present a 3D microreactor capable of maintaining metabolically active HepG2/C3A spheroids for over 28 days in vitro under stable oxygen gradients mimicking the in vivo microenvironment. Mitochondrial respiration was monitored using two-frequency phase modulation of phosphorescent microprobes embedded in the tissue. Phase modulation is focus independent and unaffected by cell death or migration. This sensitive measurement of oxygen dynamics revealed important information on the drug mechanism of action and transient subthreshold effects. Specifically, exposure to antiarrhythmic agent, amiodarone, showed that both respiration and the time to onset of mitochondrial damage were dose dependent showing a TC50 of 425 μm. Analysis showed significant induction of both phospholipidosis and microvesicular steatosis during long-term exposure. Importantly, exposure to widely used analgesic, acetaminophen, caused an immediate, reversible, dose-dependent loss of oxygen uptake followed by a slow, irreversible, dose-independent death, with a TC50 of 12.3 mM. Transient loss of mitochondrial respiration was also detected below the threshold of acetaminophen toxicity. The phenomenon was repeated in HeLa cells that lack CYP2E1 and 3A4, and was blocked by preincubation with ascorbate and TMPD. These results mark the importance of tracing toxicity effects over time, suggesting a NAPQI-independent targeting of mitochondrial complex III might be responsible for acetaminophen toxicity in extrahepatic tissues.
AB - Prediction of drug-induced toxicity is complicated by the failure of animal models to extrapolate human response, especially during assessment of repeated dose toxicity for cosmetic or chronic drug treatments. In this work, we present a 3D microreactor capable of maintaining metabolically active HepG2/C3A spheroids for over 28 days in vitro under stable oxygen gradients mimicking the in vivo microenvironment. Mitochondrial respiration was monitored using two-frequency phase modulation of phosphorescent microprobes embedded in the tissue. Phase modulation is focus independent and unaffected by cell death or migration. This sensitive measurement of oxygen dynamics revealed important information on the drug mechanism of action and transient subthreshold effects. Specifically, exposure to antiarrhythmic agent, amiodarone, showed that both respiration and the time to onset of mitochondrial damage were dose dependent showing a TC50 of 425 μm. Analysis showed significant induction of both phospholipidosis and microvesicular steatosis during long-term exposure. Importantly, exposure to widely used analgesic, acetaminophen, caused an immediate, reversible, dose-dependent loss of oxygen uptake followed by a slow, irreversible, dose-independent death, with a TC50 of 12.3 mM. Transient loss of mitochondrial respiration was also detected below the threshold of acetaminophen toxicity. The phenomenon was repeated in HeLa cells that lack CYP2E1 and 3A4, and was blocked by preincubation with ascorbate and TMPD. These results mark the importance of tracing toxicity effects over time, suggesting a NAPQI-independent targeting of mitochondrial complex III might be responsible for acetaminophen toxicity in extrahepatic tissues.
KW - Acetaminophen/metabolism
KW - Activation, Metabolic
KW - Amiodarone/metabolism
KW - Analgesics, Non-Narcotic/metabolism
KW - Anti-Arrhythmia Agents/metabolism
KW - Biomarkers/metabolism
KW - Bioreactors
KW - Cellular Microenvironment
KW - Chemical and Drug Induced Liver Injury/enzymology
KW - Coculture Techniques
KW - Cytochrome P-450 CYP2E1/metabolism
KW - Dose-Response Relationship, Drug
KW - Equipment Design
KW - Hep G2 Cells
KW - Hepatocytes/drug effects
KW - Humans
KW - Lab-On-A-Chip Devices
KW - Mitochondria, Liver/drug effects
KW - Oxygen Consumption
KW - Spheroids, Cellular
KW - Time Factors
UR - http://www.scopus.com/inward/record.url?scp=84930370310&partnerID=8YFLogxK
U2 - 10.1007/s00204-015-1537-2
DO - 10.1007/s00204-015-1537-2
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C2 - 26041127
SN - 0340-5761
VL - 90
SP - 1181
EP - 1191
JO - Archives of Toxicology
JF - Archives of Toxicology
IS - 5
ER -