Effects of diphenylaminoethanol and lidocaine on central inhibition

International journal of neuropharmacology Pub Date : 1969-05-01 DOI:10.1016/0028-3908(69)90042-2

Ronald D. Huffman, George K.W. Yim

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引用次数: 12

Abstract

In normal cats, 1, 1-diphenyl-2-aminoethanol (DPAE) caused ataxia, intentional tremors, and convulsions whereas lidocaine caused ataxia and convulsions but no tremors. In decerebrate cats, DPAE markedly inhibited cerebellar disfacilitation of spinal monosynaptic reflexes, slightly depressed reticular inhibition and had no effect on direct inhibition. The unconditioned monosynaptic reflex was facilitated by low doses and depressed by high doses of DPAE. DPAE did not affect reticular facilitation indicating that DPAE did not block cerebellar disfacilitation by depressing the facilitatory input to lower motoneurones. Lidocaine markedly reduced cerebellar disfacilitation and also reduced reticular and presynaptic inhibition as well as pressor and facilitatory responses.

It is concluded that the tremors and ataxia of DPAE are manifestations of the preferential blockade of cerebellar disfacilitation, and that this action of DPAE may take place at the inhibitory synapses of cerebellar Purkinje cells on neuronal systems responsible for the tonic excitatory input to lower motoneurones.

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二苯胺乙醇和利多卡因对中枢抑制的影响

在正常猫中，1,1 -二苯基-2-氨基乙醇(DPAE)引起共济失调、故意震颤和抽搐，而利多卡因引起共济失调和抽搐，但没有震颤。在失脑猫中，DPAE显著抑制小脑脊髓单突触反射的失易化，轻微抑制网状抑制，对直接抑制无影响。低剂量DPAE促进单突触反射，高剂量DPAE抑制单突触反射。DPAE不影响网状易化，表明DPAE不通过抑制向下运动神经元的易化输入来阻断小脑易化。利多卡因显著减少小脑疏通，也减少网状和突触前抑制以及加压和促进反应。结果表明，DPAE的震颤和共济失调是小脑失易化优先阻断的表现，DPAE的作用可能发生在负责向下运动神经元提供紧张性兴奋输入的小脑浦肯野细胞的抑制突触上。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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International journal of neuropharmacology

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