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将神经性有机磷化合物局部应用于母鸡坐骨神经:对神经病靶酯酶的抑制作用及周围神经损伤

Local application of neuropathic organophosphorus compounds to hen sciatic nerve: inhibition of neuropathy target esterase and peripheral neurological impairments.

作者信息

Carrera V, Barril J, Mauricio M, Pellín M, Vilanova E

机构信息

Department of Neurochemistry, University of Alicante, Spain.

出版信息

Toxicol Appl Pharmacol. 1992 Dec;117(2):218-25. doi: 10.1016/0041-008x(92)90240-s.

Abstract

Diisopropyl phosphorofluoridate (DFP), mipafox, cresylsaligenyl phosphate, and phenylsaligenyl phosphate were applied to a 1.5-cm segment of the common trunk of the sciatic nerve in adult hens. At doses of 18-182 micrograms mipafox and 9-110 micrograms DFP, inhibition of neuropathy target esterase (NTE) for the treated segment was over 80%, whereas for the adjacent distal and proximal segments inhibition was under 40%, 15 min after application. NTE was not affected in the peripheral distal terminations arising from the common sciatic nerve (peroneal branches), contralateral sciatic nerve, brain, and spinal cord. A 24-hr study suggested a displacement of the activity-free region toward more distal segments of the nerve. All animals treated with 55 and 110 micrograms DFP or 110 micrograms mipafox lost a characteristic avian retraction reflex in the treated leg 9-15 days after dosing, suggesting peripheral neurological alterations. Only hens dosed at the maximum dose in both extremities presented alterations in motility (Grade 1 or 2 on a 0-8 scale), suggesting no significant central nervous system alterations. Electron microscopy of peroneal branches showed axon swelling and accumulation of smooth endoplasmic reticulum similar to animals dosed systemically (s.c.) with 1-2 mg/kg DFP. The branches also contained granular and electron-dense materials, as well as some intraaxonal and intramyelinic vacuolization. Clinical effects were not observed in animals protected with a 30 mg/kg (s.c.) dose of phenylmethanesulphonyl fluoride. It is concluded that the peripheral neurological effects of local dosing correlate with the specific modification of NTE in a segment of sciatic nerve and that the axon is a more likely target than the perikaryon or nerve terminal in the triggering mechanism of this axonopathy.

摘要

将二异丙基氟磷酸酯(DFP)、丙氟磷、甲酚基磷酸水杨酯和苯基磷酸水杨酯应用于成年母鸡坐骨神经总干1.5厘米长的节段。在丙氟磷剂量为18 - 182微克、DFP剂量为9 - 110微克时,给药后15分钟,处理节段的神经病靶酯酶(NTE)抑制率超过80%,而相邻的远端和近端节段抑制率低于40%。坐骨神经总干发出的外周远端终末(腓神经分支)、对侧坐骨神经、脑和脊髓中的NTE未受影响。一项24小时的研究表明,无活性区域向神经更远端节段移位。所有用55和110微克DFP或110微克丙氟磷处理的动物在给药后9 - 15天,处理腿失去了特征性的禽类回缩反射,提示外周神经改变。只有在双下肢均给予最大剂量药物的母鸡出现运动改变(0 - 8级为1或2级),提示无明显中枢神经系统改变。腓神经分支的电子显微镜检查显示轴突肿胀和平滑内质网积聚,类似于经皮下给予1 - 2毫克/千克DFP的动物。分支中还含有颗粒状和电子致密物质,以及一些轴突内和髓鞘内空泡化。用30毫克/千克(皮下)剂量的苯甲磺酰氟保护的动物未观察到临床效应。结论是,局部给药的外周神经效应与坐骨神经节段中NTE的特异性改变相关,并且在这种轴索性神经病的触发机制中,轴突比核周体或神经末梢更可能是靶点。

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