Literature DB >> 10873710

Maturation-dependent effects of chlorpyrifos and parathion and their oxygen analogs on acetylcholinesterase and neuronal and glial markers in aggregating brain cell cultures.

F Monnet-Tschudi1, M G Zurich, B Schilter, L G Costa, P Honegger.   

Abstract

An in vitro model, the aggregating brain cell culture of fetal rat telencephalon, has been used to study the maturation-dependent sensitivity of brain cells to two organophosphorus pesticides (OPs), chlorpyrifos and parathion, and to their oxon derivatives. Immature (DIV 5-15) or differentiated (DIV 25-35) brain cells were treated continuously for 10 days. Acetylcholinesterase (AChE) inhibitory potency for the OPs was compared to that of eserine (physostigmine), a reversible AChE inhibitor. Oxon derivatives were more potent AChE inhibitors than the parent compounds, and parathion was more potent than chlorpyrifos. No maturation-dependent differences for AChE inhibition were found for chlorpyrifos and eserine, whereas for parathion and paraoxon there was a tendency to be more effective in immature cultures, while the opposite was true for chlorpyrifos-oxon. Toxic effects, assessed by measuring protein content as an index of general cytotoxicity, and various enzyme activities as cell-type-specific neuronal and glial markers (ChAT and GAD, for cholinergic and GABAergic neurons, respectively, and GS and CNP, for astrocytes and oligodendrocytes, respectively) were only found at more than 70% of AChE inhibition. Immature compared to differentiated cholinergic neurons appeared to be more sensitive to OP treatments. The oxon derivates were found to be more toxic on neurons than the parent compounds, and chlorpyrifos was more toxic than parathion. Eserine was not neurotoxic. These results indicate that inhibition of AChE remains the most sensitive macromolecular target of OP exposure, since toxic effects were found at concentrations in which AChE was inhibited. Furthermore, the compound-specific reactions, the differential pattern of toxicity of OPs compared to eserine, and the higher sensitivity of immature brain cells suggest that the toxic effects and inhibition of AChE are unrelated.

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Year:  2000        PMID: 10873710     DOI: 10.1006/taap.2000.8934

Source DB:  PubMed          Journal:  Toxicol Appl Pharmacol        ISSN: 0041-008X            Impact factor:   4.219


  27 in total

1.  Prenatal exposure of guinea pigs to the organophosphorus pesticide chlorpyrifos disrupts the structural and functional integrity of the brain.

Authors:  Roger J Mullins; Su Xu; Edna F R Pereira; Joseph D Pescrille; Spencer W Todd; Jacek Mamczarz; Edson X Albuquerque; Rao P Gullapalli
Journal:  Neurotoxicology       Date:  2015-02-19       Impact factor: 4.294

2.  Developmental neurotoxicity of organophosphates targets cell cycle and apoptosis, revealed by transcriptional profiles in vivo and in vitro.

Authors:  Theodore A Slotkin; Frederic J Seidler
Journal:  Neurotoxicol Teratol       Date:  2011-12-28       Impact factor: 3.763

3.  Early postnatal parathion exposure in rats causes sex-selective cognitive impairment and neurotransmitter defects which emerge in aging.

Authors:  Edward D Levin; Olga A Timofeeva; Liwei Yang; Ann Petro; Ian T Ryde; Nicola Wrench; Frederic J Seidler; Theodore A Slotkin
Journal:  Behav Brain Res       Date:  2009-12-17       Impact factor: 3.332

4.  Consumption of a high-fat diet in adulthood ameliorates the effects of neonatal parathion exposure on acetylcholine systems in rat brain regions.

Authors:  Theodore A Slotkin; T Leon Lassiter; Ian T Ryde; Nicola Wrench; Edward D Levin; Frederic J Seidler
Journal:  Environ Health Perspect       Date:  2009-02-03       Impact factor: 9.031

5.  Comparative developmental neurotoxicity of organophosphates in vivo: transcriptional responses of pathways for brain cell development, cell signaling, cytotoxicity and neurotransmitter systems.

Authors:  Theodore A Slotkin; Frederic J Seidler
Journal:  Brain Res Bull       Date:  2007-01-25       Impact factor: 4.077

6.  Chlorpyrifos and chlorpyrifos-oxon inhibit axonal growth by interfering with the morphogenic activity of acetylcholinesterase.

Authors:  Dongren Yang; Angela Howard; Donald Bruun; Mispa Ajua-Alemanj; Cecile Pickart; Pamela J Lein
Journal:  Toxicol Appl Pharmacol       Date:  2007-11-17       Impact factor: 4.219

7.  The sea urchin embryo, an invertebrate model for mammalian developmental neurotoxicity, reveals multiple neurotransmitter mechanisms for effects of chlorpyrifos: therapeutic interventions and a comparison with the monoamine depleter, reserpine.

Authors:  Gennady A Buznikov; Lyudmila A Nikitina; Ljubisa M Rakić; Ivan Milosević; Vladimir V Bezuglov; Jean M Lauder; Theodore A Slotkin
Journal:  Brain Res Bull       Date:  2007-07-06       Impact factor: 4.077

8.  Developmental neurotoxic effects of chlorpyrifos on acetylcholine and serotonin pathways in an avian model.

Authors:  Theodore A Slotkin; Frederic J Seidler; Ian T Ryde; Joseph Yanai
Journal:  Neurotoxicol Teratol       Date:  2008-03-18       Impact factor: 3.763

9.  Repeated gestational exposure of mice to chlorpyrifos oxon is associated with paraoxonase 1 (PON1) modulated effects in maternal and fetal tissues.

Authors:  Toby B Cole; Wan-Fen Li; Aila L Co; Ariel M Hay; James W MacDonald; Theo K Bammler; Federico M Farin; Lucio G Costa; Clement E Furlong
Journal:  Toxicol Sci       Date:  2014-07-28       Impact factor: 4.849

10.  Inorganic lead (Pb)- and mercury (Hg)-induced neuronal cell death involves cytoskeletal reorganization.

Authors:  Woo-Sung Choi; Su-Jin Kim; Jin Suk Kim
Journal:  Lab Anim Res       Date:  2011-09-30
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