Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos,Chlorpyrifos Oxon,and Diazinon

Ruth R.Jameson; Frederic J.Seidler; Theodore A.Slotkin

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Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos,Chlorpyrifos Oxon,and Diazinon

机译：乙酰胆碱酯酶剪接变体在有机磷酸盐发育神经毒性中的非酶功能：毒死rif，毒死Ox和二嗪农

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BACKGROUND: Organophosphate pesticides affect mammalian brain development through mechanisms separable from the inhibition of acetylcholinesterase (AChE) enzymatic activity and resultant cholinergic hyperstimulation.In the brain,AChE has two catalytically similar splice variants with distinct functions in development and repair.The rare,read-through isoform,AChE-R,is preferentially induced by injury and appears to promote repair and protect against neurodegeneration.Overexpression of the more abundant,synaptic isoform,AChE-S,enhances neurotoxicity.OBJECTIVES: We exposed differentiating PC12 cells,a model for developing neurons,to 30 mu M chlorpyrifos (CPF) or diazinon (DZN),or CPF oxon,the active metabolite that irreversibly inhibits AChE enzymatic activity,in order to determine whether they differentially induce the formation of AChE-S as a mechanistic predictor of developmental neurotoxicity.We then administered CPF or DZN to neonatal rats on postnatal days 1-4 using daily doses spanning the threshold for AChE inhibition (0-20%);we then evaluated AChE gene expression in forebrain and brainstem on postnatal day 5. RESULTS: In PC12 cells,after 48 hr of exposure,CPF,CPF oxon,and DZN enhanced gene expression for AChE-R by about 20%,whereas CPF and DZN,but not CPF oxon,increased AChE-S expression by 20-40%.Thus,despite the fact that CPF oxon is a much more potent AChE inhibitor,it is the native compound (CPF) that induces expression of the neurotoxic AChE-S isoform.For in vivo exposures,1 mg/kg CPF had little or no effect,but 0.5 or 2 mg/kg DZN induced both AChE-R and AChE-S,with a greater effect in males.CONCLUSIONS: Our results indicate that nonenzymatic functions of AChE variants may participate in and be predictive of the relative developmental neurotoxicity of organophosphates,and that the various organophosphates differ in the degree to which they activate this mechanism.

机译：背景：有机磷酸酯农药通过与抑制乙酰胆碱酯酶（AChE）的酶活性和由此产生的胆碱能过度刺激分离的机制影响哺乳动物的大脑发育。在大脑中，AChE具有两个催化相似的剪接变体，在发育和修复中具有不同的功能。 AChE-R亚型通过损伤被优先诱导，并似乎促进修复和保护神经变性。更丰富的突触亚型AChE-S的过表达增强神经毒性。目的：我们暴露出分化的PC12细胞，这是一种发育模型神经元对30μM毒死rif（CPF）或二嗪农（DZN）或CPF oxon的活性，不可逆地抑制AChE酶活性的活性代谢物，以确定它们是否以差异方式诱导AChE-S的形成，作为发育的机械预测因子神经毒性。然后在出生后的第1-4天以每天的剂量范围向新生大鼠施用CPF或DZN设定AChE抑制阈值（0-20％）;然后在出生后第5天评估前脑和脑干中AChE基因的表达。结果：在PC12细胞中，暴露48小时后，CPF，CPF oxon和DZN增强了基因表达对于AChE-R大约20％，而CPF和DZN而不是CPF oxon使AChE-S表达提高20-40％。因此，尽管CPF oxon是更有效的AChE抑制剂，但它是天然的化合物（CPF）诱导神经毒性AChE-S亚型的表达。对于体内暴露，1 mg / kg CPF几乎没有影响，但0.5或2 mg / kg DZN诱导了AChE-R和AChE-S的共同作用。结论：我们的结果表明，AChE变体的非酶功能可能参与并预测了有机磷酸酯的相对发育神经毒性，并且各种有机磷酸酯在激活这种机制的程度上也有所不同。

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《Environmental health perspectives.》 |2007年第1期|共6页
作者
Ruth R.Jameson; Frederic J.Seidler; Theodore A.Slotkin;
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中图分类环境科学、安全科学;
关键词
acetylcholinesterase; brain development; chlorpyrifos; diazinon; organophosphate insecticides; PC12 cells.;

机译：乙酰胆碱酯酶;脑发育;毒死rif;二嗪农;有机磷酸酯杀虫剂;PC12细胞。;

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1. Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos,Chlorpyrifos Oxon,and Diazinon [J] . Ruth R.Jameson, Frederic J.Seidler, Theodore A.Slotkin Environmental health perspectives. . 2007,第1期

机译：乙酰胆碱酯酶剪接变体在有机磷酸盐发育神经毒性中的非酶功能：毒死rif，毒死Ox和二嗪农
2. An evaluation of the inhibition of human butyrylcholinesterase and acetylcholinesterase by the organophosphate chlorpyrifos oxon. [J] . Shenouda J, Green P, Sultatos L Toxicology and Applied Pharmacology . 2009,第2期

机译：评价有机磷酸毒死py对人丁酰胆碱酯酶和乙酰胆碱酯酶的抑制作用。
3. Concentration-dependent interactions of the organophosphates chlorpyrifos oxon and methyl paraoxon with human recombinant acetylcholinesterase. [J] . Kaushik R, Rosenfeld CA, Sultatos LG Toxicology and Applied Pharmacology . 2007,第2期

机译：有机磷酸盐毒死和甲基对氧磷与人重组乙酰胆碱酯酶的浓度依赖性相互作用。
4. Effects of an Educational Intervention on Organophosphate Pesticides in the Risk Perception and Chlorpyrifos, Diazinon and Parathion Metabolites Levels in Chilean Rural Schoolchildren [C] . Maria Teresa Munoz-Quezada, Boris A. Lucero, Veronica Iglesias, Joint annual meeting of the International Society of Exposure Science and the International Society for Environmental Epidemiology . 2018

机译：教育干预对智利农村学龄儿童风险感知和毒死rif，二嗪农和对硫磷代谢物含量中有机磷农药的影响
5. Developmental neurotoxicity of chlorpyrifos: Effects on the serotonergic system. [D] . Aldridge, Justin Edward. 2005

机译：毒死rif的发育神经毒性：对血清素能系统的影响。
6. Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos Chlorpyrifos Oxon and Diazinon [O] . Ruth R. Jameson, Frederic J. Seidler, Theodore A. Slotkin 2007

机译：乙酰胆碱酯酶剪接变体在有机磷酸盐发育神经毒性中的非酶功能：毒死rif毒死Ox和二嗪农
7. Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos, Chlorpyrifos Oxon, and Diazinon [O] . Jameson, Ruth R., Seidler, Frederic J., Slotkin, Theodore A. 2006

机译：乙酰胆碱酯酶剪接变体在有机磷酸盐发育神经毒性中的非酶功能：毒死rif，毒死Ox和二嗪农
8. Relative Inhibitory Potencies of Chlorpyrifos Oxon, Chlorpyrifos Methyl Oxon, and Mipafox for Acetylcholinesterase Versus Neuropathy Target Esterase [R] . Kropp, T. J. , Richardson, R. J. 2003

机译：毒死蜱，毒死蜱甲基氧杂和mipafox对乙酰胆碱酯酶与神经病变靶蛋白酶的相对抑制作用

Nonenzymatic Functions of Acetylcholinesterase Splice Variants in the Developmental Neurotoxicity of Organophosphates: Chlorpyrifos,Chlorpyrifos Oxon,and Diazinon

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