This study investigates the neurodevelopmental toxicity of rotenone, a mitochondrial Complex I inhibitor, using a 3D human iPSC-derived brain model known as BrainSpheres. By exposing spheroids at various stages of neural differentiation to rotenone, researchers observed dose- and time-dependent impacts on mitochondrial function, reactive oxygen species (ROS) production, and gene expression. Findings showed increased vulnerability during early differentiation, particularly among dopaminergic neurons, supporting the use of BrainSpheres as a model to assess human-specific developmental neurotoxicity (DNT).
Researchers generated BrainSpheres from neural progenitor cells derived from human induced pluripotent stem cells (iPSCs). Differentiated over 2, 4, and 8 weeks, BrainSpheres were exposed to varying concentrations of rotenone for up to 48 hours. A suite of assays—including cell viability, ROS, mitochondrial activity (MitoTracker), immunofluorescence, transcriptomics (microarray), and metabolomics (LC-MS)—was conducted to evaluate cellular and molecular responses.
The study demonstrates that rotenone has a pronounced neurotoxic effect on human brain development in vitro, particularly affecting early-stage neurons and dopaminergic populations. BrainSpheres effectively mimic critical aspects of brain development, providing a valuable tool for screening potential neurodevelopmental toxicants. Results highlight the importance of incorporating human-relevant models in toxicology to better understand environmental risk factors and support regulatory alternatives to animal testing.
Pamies D, Block K, Lau P, et al. Rotenone exerts developmental neurotoxicity in a human brain spheroid model. Toxicol Appl Pharmacol. 2018;354:101–114. doi:10.1016/j.taap.2018.02.003
