Slotkin Theodore A, Bodwell Bethany E, Ryde Ian T, Levin Edward D, Seidler Frederic J
Department of Pharmacology and Cancer Biology, Duke University Medical Center, Durham, North Carolina 27710, USA.
Environ Health Perspect. 2008 Oct;116(10):1308-14. doi: 10.1289/ehp.11451. Epub 2008 May 19.
Organophosphates elicit developmental neurotoxicity through multiple mechanisms other than their shared property as cholinesterase inhibitors. Accordingly, these agents may differ in their effects on specific brain circuits.
We gave parathion to neonatal rats [postnatal days (PNDs) 1-4], at daily doses of 0.1 or 0.2 mg/kg, spanning the threshold for barely detectable cholinesterase inhibition and systemic effects.
We assessed neurochemical indices related to the function of acetylcholine (ACh) synapses (choline acetyltransferase, presynaptic high-affinity choline transporter, nicotinic cholinergic receptors) in brain regions comprising all the major ACh projections, with determinations carried out from adolescence to adulthood (PNDs 30, 60, and 100).
Parathion exposure elicited lasting alterations in ACh markers in the frontal/parietal cortex, temporal/occipital cortex, midbrain, hippocampus, and striatum. In cerebrocortical areas, midbrain, and hippocampus, effects in males were generally greater than in females, whereas in the striatum, females were targeted preferentially. Superimposed on this general pattern, the cerebrocortical effects showed a nonmonotonic dose-response relationship, with regression of the defects at the higher parathion dose; this relationship has been seen also after comparable treatments with chlorpyrifos and diazinon and likely represents the involvement of cholinesterase-related actions that mask or offset the effects of lower doses.
Neonatal exposure to parathion, at doses straddling the threshold for cholinesterase inhibition, compromises indices of ACh synaptic function in adolescence and adulthood. Differences between the effects of parathion compared with chlorpyrifos or diazinon and the non-monotonic dose-effect relationships reinforce the conclusion that various organophosphates diverge in their effects on neurodevelopment, unrelated to their anticholinesterase actions.
有机磷酸酯通过多种机制引发发育性神经毒性,而非仅通过其作为胆碱酯酶抑制剂的共同特性。因此,这些药剂对特定脑回路的影响可能有所不同。
我们给新生大鼠[出生后第(PND)1 - 4天]每日腹腔注射0.1或0.2mg/kg的对硫磷,该剂量跨越了几乎检测不到胆碱酯酶抑制和全身效应的阈值。
我们评估了与乙酰胆碱(ACh)突触功能相关的神经化学指标(胆碱乙酰转移酶、突触前高亲和力胆碱转运体、烟碱型胆碱能受体),这些指标来自包含所有主要ACh投射的脑区,并在青春期至成年期(PND 30、60和100)进行测定。
对硫磷暴露导致额叶/顶叶皮质、颞叶/枕叶皮质、中脑、海马体和纹状体中ACh标记物的持久改变。在脑皮质区域、中脑和海马体中,雄性大鼠的影响通常大于雌性,而在纹状体中,雌性大鼠更易受到影响。在此总体模式之上,脑皮质效应呈现非单调剂量反应关系,在较高对硫磷剂量下缺陷有所消退;在使用毒死蜱和二嗪农进行类似处理后也观察到这种关系,这可能代表胆碱酯酶相关作用的参与,掩盖或抵消了较低剂量的影响。
新生大鼠在胆碱酯酶抑制阈值附近暴露于对硫磷,会损害青春期和成年期ACh突触功能指标。与毒死蜱或二嗪农相比,对硫磷效应的差异以及非单调剂量效应关系强化了以下结论:各种有机磷酸酯对神经发育的影响不同,与其抗胆碱酯酶作用无关。
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