Upscaling biological complexity to boost neuronal and oligodendroglia maturation and improve in vitro developmental neurotoxicity (DNT) evaluation

Nunes, Carolina; Gorczyca, Gabriela; Gyves, Emilio Mendoza-de; Ponti, Jessica; Bogni, Alessia; Carpi, Donatella; Bal‐Price, Anna; Pistollato, Francesca

doi:10.1016/j.reprotox.2022.03.017

Cited by 7 publications

(11 citation statements)

References 78 publications

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“…The use of in silico methods such as PBK modelling serves as a predictive tool for any substance systemic exposure and could be valuable to support risk assessment when data are sparse, such as in pregnant women ( Coppola et al, 2021 ). In this work, we performed QIVIVE to evaluate the quantitative predictive value of an vitro test system for DNT effects which was assumed to be promising in this respect ( Pistollato et al, 2020 ; Pistollato et al, 2021 ; Nunes et al, 2022 ), using non-acetyl cholinesterase-dependent markers in hiPSC-derived neuronal/glial cell model.…”

Section: Discussionmentioning

confidence: 99%

Prediction of in vivo prenatal chlorpyrifos exposure leading to developmental neurotoxicity in humans based on in vitro toxicity data by quantitative in vitro–in vivo extrapolation

et al. 2023

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Introduction: Epidemiological studies in children suggested that in utero exposure to chlorpyrifos (CPF), an organophosphate insecticide, may cause developmental neurotoxicity (DNT). We applied quantitative in vitro–in vivo extrapolation (QIVIVE) based on in vitro concentration and non-choline esterase-dependent effects data combined with Benchmark dose (BMD) modelling to predict oral maternal CPF exposure during pregnancy leading to fetal brain effect concentration. By comparing the results with data from epidemiological studies, we evaluated the contribution of the in vitro endpoints to the mode of action (MoA) for CPF-induced DNT.Methods: A maternal-fetal PBK model built in PK-Sim® was used to perform QIVIVE predicting CPF concentrations in a pregnant women population at 15 weeks of gestation from cell lysate concentrations obtained in human induced pluripotent stem cell-derived neural stem cells undergoing differentiation towards neurons and glia exposed to CPF for 14 days. The in vitro concentration and effect data were used to perform BMD modelling.Results: The upper BMD was converted into maternal doses which ranged from 3.21 to 271 mg/kg bw/day. Maternal CPF blood levels from epidemiological studies reporting DNT findings in their children were used to estimate oral CPF exposure during pregnancy using the PBK model. It ranged from 0.11 to 140 μg/kg bw/day.Discussion: The effective daily intake doses predicted from the in vitro model were several orders of magnitude higher than exposures estimated from epidemiological studies to induce developmental non-cholinergic neurotoxic responses, which were captured by the analyzed in vitro test battery. These were also higher than the in vivo LOEC for cholinergic effects. Therefore, the quantitative predictive value of the investigated non-choline esterase-dependent effects, although possibly relevant for other chemicals, may not adequately represent potential key events in the MoA for CPF-associated DNT.

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Section: Discussionmentioning

confidence: 99%

Prediction of in vivo prenatal chlorpyrifos exposure leading to developmental neurotoxicity in humans based on in vitro toxicity data by quantitative in vitro–in vivo extrapolation

et al. 2023

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“…P3143) (0.1% solution in sodium-tetra-borate buffer) and laminin (mouse protein, 10 µg/mL) coated 24-well microelectrode array (MEA) plates (24-well glass MEA plate (24W300/30 G-288) V.232, from Multi-Channel System) in 100 µL volume, and after 20 min, 400 µL medium/well was added (50,000 cells/well in 0.5 mL). Further details about model characterization are provided in our previous studies [2] , [47] .…”

Section: Methodsmentioning

confidence: 99%

“…In our recently published paper, we demonstrated that human iPSC-derived neuronal cultures are suitable to measure neurotransmitter release [45] . Therefore, in the present study, we applied this HPLC technology to measure the release of neurotransmitters in a previously well characterized hiPSC-derived NSC culture undergoing differentiation towards a mixed population of neurons and glia [2] , [46] , [47] . We assessed glutamate release in control cultures and upon exposure to DL-threo-β-Hydroxyaspartic acid (DL-TBOA, a non-transportable glutamate uptake inhibitor [48] ), 4-aminopyridine (4-AP, which induces action potential-like membrane depolarization by blocking voltage-gated K + -channels, causing in vitro release of glutamate, [49] , [50] ), bafilomycin A1 (Bafilo, a specific and potent inhibitor of vacuolar-type H + -ATPase required for the exocytotic vesicle loading with glutamate [51] , [52] , [53] ), or a combination of 4-AP and Bafilo.…”

Section: Introductionmentioning

confidence: 99%

Assessment of neurotransmitter release in human iPSC-derived neuronal/glial cells: a missing in vitro assay for regulatory developmental neurotoxicity testing

Cervetto

Pistollato

Amato

et al. 2023

Reproductive Toxicology

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“…For example, it is hard to develop a co-culture of neurons and oligodendrocytes with active myelination, but differentiation towards myelinating oligodendrocytes can easily be achieved using 3D neurospheres, compensating for the limitation of using 2D monolayer cultures [57]. These 3D neurospheres enable robust differentiation towards both neuronal and glial cell populations, including myelination and formation of more mature neuronal network activity when compared to 2D monolayer culture [19,57,63].…”

Section: Complexity Of the Applied Model: 2d Versus 3dmentioning

confidence: 99%

“…Clearly, the selection of a 2D versus a 3D model is likely to affect the results obtained. For example, 2D models are still more suitable to assess neuronal functionality by analysis of spontaneous electrical activity using traditional multielectrode array platform [63]. However, the fast development of new technologies, and increasing number of new bioengineered devices more suitable for electrophysiological recordings in 3D [71][72][73][74] might change that.…”

Section: Complexity Of the Applied Model: 2d Versus 3dmentioning

confidence: 99%

Quality criteria for in vitro human pluripotent stem cell-derived models of tissue-based cells

Pistollato

Bal‐Price

Coecke

et al. 2022

Reproductive Toxicology

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Upscaling biological complexity to boost neuronal and oligodendroglia maturation and improve in vitro developmental neurotoxicity (DNT) evaluation

Cited by 7 publications

References 78 publications

Prediction of in vivo prenatal chlorpyrifos exposure leading to developmental neurotoxicity in humans based on in vitro toxicity data by quantitative in vitro–in vivo extrapolation

Prediction of in vivo prenatal chlorpyrifos exposure leading to developmental neurotoxicity in humans based on in vitro toxicity data by quantitative in vitro–in vivo extrapolation

Assessment of neurotransmitter release in human iPSC-derived neuronal/glial cells: a missing in vitro assay for regulatory developmental neurotoxicity testing

Quality criteria for in vitro human pluripotent stem cell-derived models of tissue-based cells

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