Developmental neurotoxicity of chlorpyrifos: what is the vulnerable period?

Qiao, Dan; Seidler, Frederic J.; Padilla, Stephanie; Slotkin, Theodore A.

doi:10.1289/ehp.021101097

Cited by 119 publications

(116 citation statements)

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“…Systemic toxicity of CPF. As reported previously (Garcia et al 2002;Qiao et al 2002), the threshold for CPF-induced impairment of maternal growth was 5 mg/kg with treatment on either GD9-12 or GD17-20, but fetal brain growth was unaffected even at the highest doses (data not shown). Neither the early nor the late treatment paradigm affected the number of fetuses or fetal viability.…”

Section: Resultssupporting

confidence: 82%

“…In both periods, CPF elicits mitotic abnormalities, apoptosis, and architectural anomalies in the developing brain at exposures that are not otherwise embryotoxic Roy et al 1998;White et al 2002). At lower exposure levels, CPF-induced damage is not immediately apparent, but synaptic and functional abnormalities appear later, in adolescence and adulthood (Levin et al 2002;Qiao et al 2002Qiao et al , 2003. Thus, if the production of cAMP is involved in the adverse effects of CPF on brain development, effects on the AC signaling pathway should be evident immediately upon exposure to these lower exposures, preceding the delayed-onset anomalies.…”

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confidence: 99%

“…Because the treatments were given to the dams, only one fetus was used from each dam, so the number of determinations represents the number of dams. The fetuses were derived from the same litters as those used in two previous studies on cell damage and cholinergic biomarkers; therefore effects on cholinesterase activity, maternal and fetal body weights, and other litter characteristics have been published elsewhere (Garcia et al 2002;Qiao et al 2002).…”

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confidence: 99%

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Developmental neurotoxicity elicited by gestational exposure to chlorpyrifos: when is adenylyl cyclase a target?

Meyer

Seidler

Cousins

et al. 2003

Environ Health Perspect

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The developmental neurotoxicity of chlorpyrifos (CPF) involves mechanisms over and above cholinesterase inhibition. In the present study, we evaluated the effects of gestational CPF exposure on the adenylyl cyclase (AC) signaling cascade, which regulates the production of cyclic AMP, a major controller of cell replication and differentiation. In addition to basal AC activity, we assessed the AC response to direct enzymatic stimulants [forskolin, manganese (Mn 2+ )]; the response to isoproterenol, which activates signaling through β-adrenoceptors (βARs); and the concentration of βAR binding sites. CPF administered to pregnant rats on gestational days (GD) 9-12 elicited little or no change in any components of AC activity or βARs. However, shifting the treatment window to GD17-20 produced regionally selective augmentation of AC activity. In the brainstem, the response to forskolin or Mn 2+ was markedly stimulated by doses at or below the threshold for observable toxicity of CPF or for inhibition of fetal brain cholinesterase, whereas comparable effects were seen in the forebrain only at higher doses. In addition, low doses of CPF reduced βAR binding without impairing receptor-mediated stimulation of AC. These results indicate that signal transduction through the AC cascade is a target for CPF during a discrete developmental period in late gestation, an effect that is likely to contribute to the noncholinergic component of CPF's developmental neurotoxicity. Key words: adenylyl cyclase, β-adrenoceptor, brain development, chlorpyrifos, organophosphate insecticides.

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Section: Resultssupporting

confidence: 82%

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confidence: 99%

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confidence: 99%

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Developmental neurotoxicity elicited by gestational exposure to chlorpyrifos: when is adenylyl cyclase a target?

Meyer

Seidler

Cousins

et al. 2003

Environ Health Perspect

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“…39 Given the diversity of possible mechanisms and target tissues, the developing brain could be vulnerable to organophosphate pesticide exposure from early embryonic life into childhood. 16,[80][81][82][83][84][85] According to Slotkin, 22 the period of vulnerability to chlorpyrifos extends through the period of synaptic modeling, and this continues well into childhood and even adolescence. In the present report, both chlorpyrifos and lead exposures were assessed during the prenatal period only, which is a limitation.…”

Section: Discussionmentioning

confidence: 99%

Impact of Prenatal Chlorpyrifos Exposure on Neurodevelopment in the First 3 Years of Life Among Inner-City Children

et al. 2006

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OBJECTIVE-The purpose of this study was to investigate the impact of prenatal exposure to chlorpyrifos on 3-year neurodevelopment and behavior in a sample of inner-city minority children.METHODS-As part of an ongoing prospective cohort study in an inner-city minority population, neurotoxicant effects of prenatal exposure to chlorpyrifos were evaluated in 254 children through the first 3 years of life. This report examined cognitive and motor development at 12, 24, and 36 months (measured with the Bayley Scales of Infant Development II) and child behavior at 36 months (measured with the Child Behavior Checklist) as a function of chlorpyrifos levels in umbilical cord plasma.RESULTS-Highly exposed children (chlorpyrifos levels of >6.17 pg/g plasma) scored, on average, 6.5 points lower on the Bayley Psychomotor Development Index and 3.3 points lower on the Bayley Mental Development Index at 3 years of age compared with those with lower levels of exposure. Children exposed to higher, compared with lower, chlorpyrifos levels were also significantly more likely to experience Psychomotor Development Index and Mental Development Index delays, attention problems, attention-deficit/hyperactivity disorder problems, and pervasive developmental disorder problems at 3 years of age. CONCLUSIONS-The adjusted mean 36-month Psychomotor Development Index and MentalDevelopment Index scores of the highly and lower exposed groups differed by only 7.1 and 3.0 points, respectively, but the proportion of delayed children in the high-exposure group, compared with the low-exposure group, was 5 times greater for the Psychomotor Development Index and 2.4 times greater for the Mental Development Index, increasing the number of children possibly needing early intervention services. NIH Public Access Author ManuscriptPediatrics. Author manuscript; available in PMC 2012 July 06. As a result of heavy indoor use, largely for cockroach control, pesticide exposure is widespread among pregnant women living in New York City. [3][4][5][6][7][8] Specifically, 72% to 85% of women participating in 2 different cohort studies reported using some form of pest control during pregnancy, 3,7-9 and 46% reported using ≥1 of the higher-toxicity methods, such as exterminator sprays, can sprays, and pest bombs. 3 A survey of pest control measures conducted in 2000 and 2001 by the office of the New York State Attorney General found that 93% of New York City public housing residents applied pesticides at home and more than one half did so approximately once per week. 6 In a previous report from the present cohort, detectable levels of chlorpyrifos were found in 99.7% of personal air samples and 100% of indoor air samples from stationary residential monitors for a sample of pregnant women. 8 Chlorpyrifos was also detected in 64% to 70% of blood samples collected from mothers and newborns at delivery. Maternal levels and newborn levels were correlated strongly, which indicates that this pesticide crosses the placenta readily. 3 Since the ban, levels of chlorpyr...

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“…Although it was originally thought that these agents act solely through inhibition of cholinesterase and consequent cholinergic hyperstimulation, it is now evident that there are multiple mechanisms that contribute to neurodevelopmental abnormalities [10,17,42,73,74,77,112]. Accordingly, whereas all the organophosphates share cholinesterase as a target, they are likely to differ to a greater or lesser extent in their effects unrelated to that particular mechanism.…”

Section: Introductionmentioning

confidence: 99%

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

Slotkin

Seidler

2007

Brain Research Bulletin

193

208

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Organophosphates affect mammalian brain development through a variety of mechanisms beyond their shared property of cholinesterase inhibition. We used microarrays to characterize similarities and differences in transcriptional responses to chlorpyrifos and diazinon, assessing defined gene groupings for the pathways known to be associated with the mechanisms and/or outcomes of chlorpyrifos-induced developmental neurotoxicity. We exposed neonatal rats to daily doses of chlorpyrifos (1 mg/kg) or diazinon (1 or 2 mg/kg) on postnatal days 1-4 and evaluated gene expression profiles in brainstem and forebrain on day 5; these doses produce little or no cholinesterase inhibition. We evaluated pathways for general neural cell development, cell signaling, cytotoxicity and neurotransmitter systems, and identified significant differences for >60% of 252 genes. Chlorpyrifos elicited major transcriptional changes in genes involved in neural cell growth, development of glia and myelin, transcriptional factors involved in neural cell differentiation, cAMP-related cell signaling, apoptosis, oxidative stress, excitotoxicity, and development of neurotransmitter synthesis, storage and receptors for acetylcholine, serotonin, norepinephrine and dopamine. Diazinon had similar effects on many of the same processes but also showed major differences from chlorpyrifos. Our results buttress the idea that different organophosphates target multiple pathways involved in neural cell development but also that they deviate in key aspects that may contribute to disparate neurodevelopmental outcomes. Equally important, these pathways are compromised at exposures that are unrelated to biologically significant cholinesterase inhibition and its associated signs of systemic toxicity. The approach used here demonstrates how planned comparisons with microarrays can be used to screen for developmental neurotoxicity.

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Developmental neurotoxicity of chlorpyrifos: what is the vulnerable period?

Cited by 119 publications

References 50 publications

Developmental neurotoxicity elicited by gestational exposure to chlorpyrifos: when is adenylyl cyclase a target?

Developmental neurotoxicity elicited by gestational exposure to chlorpyrifos: when is adenylyl cyclase a target?

Impact of Prenatal Chlorpyrifos Exposure on Neurodevelopment in the First 3 Years of Life Among Inner-City Children

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

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