Evaluation of multi-well microelectrode arrays for neurotoxicity screening using a chemical training set

McConnell, Emma R.; McClain, Maxine A.; Ross, James D.; LeFew, William R.; Shafer, Timothy J.

doi:10.1016/j.neuro.2012.05.001

Cited by 150 publications

(143 citation statements)

References 36 publications

Supporting

Mentioning

124

Contrasting

Unclassified

Order By: Relevance

“…Higher concentrations of DomA (1 and 2 μM) also significantly decrease the MFR, whereas concentrations up to 0.1 μM of DomA do not cause any effect on MFR (Hogberg et al, 2011). In primary rat cortical neurons (12-22 DIV), DomA (50 μM) has been reported to reduce MFR by more than 90% (McConnell et al, 2012).…”

Section: Domoic Acid (Doma)mentioning

confidence: 88%

“…For example it has been shown that MEA-coupled neuronal cortical networks are very sensitive to pharmacological manipulation of the excitatory ionotropic glutamatergic transmission (Frega et al, 2012). MEAs can also be applied in higher throughput platforms to facilitate screening of numerous chemical compounds (McConnell et al, 2012). Excessive excitability can be also measured directly by evaluating the level of the extracellular glutamate using the enzyme-based microelectrode arrays.…”

Section: How It Is Measured or Detectedmentioning

confidence: 99%

See 1 more Smart Citation

Adverse Outcome Pathway on binding of agonists to ionotropic glutamate receptors in adult brain leading to excitotoxicity that mediates neuronal cell death, contributing to learning and memory impairment

Sachana

Munn

Bal‐Price

2016

OECD Series on Adverse Outcome Pathways

View full text Add to dashboard Cite

Section: Domoic Acid (Doma)mentioning

confidence: 88%

Section: How It Is Measured or Detectedmentioning

confidence: 99%

Adverse Outcome Pathway on binding of agonists to ionotropic glutamate receptors in adult brain leading to excitotoxicity that mediates neuronal cell death, contributing to learning and memory impairment

Sachana

Munn

Bal‐Price

2016

OECD Series on Adverse Outcome Pathways

View full text Add to dashboard Cite

“…As such, MEA recordings allow for reproducible screening of neurotoxic compounds with high sensitivity and specificity (McConnell et al, 2012;Valdivia et al, 2014;Nicolas et al, 2014). Despite the marked increase in mitochondrial activity, MEA recordings demonstrated that neuronal activity of primary cortical cultures is largely unaffected upon acute (30 min) exposure to TCP isomers, mixtures and CBDP (Figs.…”

Section: Discussionmentioning

confidence: 99%

“…Consequently, ToCP and TmCP may have different modes of action. So far, increases in MSR have been largely limited to glutamatergic agonists and GABAergic antagonists (McConnell et al, 2012;Mack et al, 2014). Since prolonged exposure to ToCP was recently reported to decrease glutamatergic signaling (Hausherr et al, 2014), it is tempting to speculate that the neurotoxicity of ToCP also involves modulation of glutamatergic receptors.…”

Section: Discussionmentioning

confidence: 99%

“…First, effects on cell viability and mitochondrial activity were assessed. Next, effects of TCPs on spontaneous neuronal electrical activity were assessed using microelectrode array (MEA) recordings as a noninvasive in vitro neurotoxicity screening method (Hogberg et al, 2011;McConnell et al, 2012;Valdivia et al, 2014;Nicolas et al, 2014). Lastly, effects on neurite outgrowth were measured as a specific, integrated measure of neurotoxicity that represents the effects of multiple underlying targets (Harrill et al, 2011).…”

Section: Tablementioning

confidence: 99%

See 1 more Smart Citation

In vitro neurotoxic hazard characterization of different tricresyl phosphate (TCP) isomers and mixtures

et al. 2017

View full text Add to dashboard Cite

A B S T R A C TExposure to tricresyl phosphates (TCPs), via for example contaminated cabin air, has been associated with health effects including the so-called aerotoxic syndrome. While TCP neurotoxicity is mainly attributed to ortho-isomers like tri-ortho-cresyl phosphate (ToCP), recent exposure and risk assessments indicate that ToCP levels in cabin air are very low. However, the neurotoxic potential of non-ortho TCP isomers and TCP mixtures is largely unknown. We therefore measured effects of exposure (up to 48 h) to different TCP isomers, mixtures and the metabolite of ToCP (CBDP: cresyl saligenin phosphate) on cell viability and mitochondrial activity, spontaneous neuronal electrical activity, and neurite outgrowth in primary rat cortical neurons.The results demonstrate that exposure to TCPs (24-48 h, up to 10 mM) increases mitochondrial activity, without affecting cell viability. Effects of acute TCP exposure (30 min) on neuronal electrical activity are limited. However, electrical activity is markedly decreased for the majority of TCPs (10 mM) following 48 h exposure. Additional preliminary data indicate that exposure to TCPs (48 h, 10 mM) did not affect the number of neurites per cell or average neurite length, except for TmCP and the analytical TCP mixture (Sigma) that induced a reduction of average neurite length.The combined neurotoxicity data demonstrate that the different TCPs, including ToCP, are roughly equipotent and a clear structure-activity relation is not apparent for the studied endpoints. The noobserved-effect-concentrations (1 mM) are well above current exposure levels indicating limited neurotoxic health risk, although exposures may have been higher in the past. Moreover, prolonged and/or repeated exposure to TCPs may exacerbate the observed neurotoxic effects, which argues for additional research.

show abstract

Overview of Electrophysiological Techniques

Wickenden

2000

CP Pharmacology

View full text Add to dashboard Cite

This unit provides an overview of the principal electrophysiological techniques commonly used for the study of ionic currents and the ion channels that mediate them. These techniques include electroencephalograms (EEGs), electrocardiograms (ECGs), single- and multiunit extracellular recording, multielectrode arrays, transepithelial recording, impedance measurements, and current-clamp, voltage-clamp, patch-clamp, and lipid bilayer recording. The unit also discusses recent advances in high-throughput, automated electrophysiological techniques for drug discovery and the use of stem cells as a tissue source.

show abstract

Evaluation of multi-well microelectrode arrays for neurotoxicity screening using a chemical training set

Cited by 150 publications

References 36 publications

Adverse Outcome Pathway on binding of agonists to ionotropic glutamate receptors in adult brain leading to excitotoxicity that mediates neuronal cell death, contributing to learning and memory impairment

Adverse Outcome Pathway on binding of agonists to ionotropic glutamate receptors in adult brain leading to excitotoxicity that mediates neuronal cell death, contributing to learning and memory impairment

In vitro neurotoxic hazard characterization of different tricresyl phosphate (TCP) isomers and mixtures

Overview of Electrophysiological Techniques

Contact Info

Product

Resources

About