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定向敏感兔视网膜神经节细胞的药理学分析

Pharmacological analysis of directionally sensitive rabbit retinal ganglion cells.

作者信息

Ariel M, Daw N W

出版信息

J Physiol. 1982 Mar;324:161-85. doi: 10.1113/jphysiol.1982.sp014105.

Abstract
  1. Cholinergic drugs were infused into the retinal circulation of the rabbit while we analysed the receptive field properties of directionally sensitive retinal ganglion cells. Physostigmine eliminated the trigger feature, directional specificity, of both types (on-centre and on-off) of these cells. In this respect the action of physostigmine (an ACh potentiator) was very like that of picrotoxin (a GABA antagonist). Therefore, a detailed analysis of the receptive field properties of directionally sensitive ganglion cells was made to analyse the effects of physostigmine and picrotoxin.2. Size specificity and radial grating inhibition were not abolished by physostigmine, but were often affected by picrotoxin. The optimal velocity in the preferred direction (as measured by maximum firing frequency) was not much changed by physostigmine, but was higher during infusion of picrotoxin. Infusion of nicotine, a depolarizing ACh agonist which increases the activity of retinal ganglion cells, revealed the presence of inhibition to movement in the null direction. The null direction response during picrotoxin started slightly later than this inhibition. The null direction response during physostigmine was weaker and started later still. Mecamylamine and dihydro-beta-erythroidine, nicrotinic receptor antagonists, totally blocked the effect of physostigmine and reduced the control light response by about half.3. From this analysis, it appears that on-off ACh release onto directionally sensitive cells provides a substantial excitation which, when potentiated by physostigmine, overcomes or outlasts the null direction GABA inhibition within the receptive field. The spatial extent of GABA inhibition is asymmetric to and larger than the spatial extent of ACh excitation. Similar pathways appear to be involved in both the on-centre and on-off directionally sensitive ganglion cells, yet the on-centre cell pathway may receive an additional input which suppresses the ACh excitation at light offset. Possible schemes for the cellular mechanism of directional sensitivity are discussed in light of these results and recent anatomical and pharmacological findings.
摘要
  1. 当我们分析方向敏感型视网膜神经节细胞的感受野特性时,将胆碱能药物注入兔子的视网膜循环。毒扁豆碱消除了这些细胞两种类型(中心-开和开-关)的触发特征,即方向特异性。在这方面,毒扁豆碱(一种乙酰胆碱增强剂)的作用与印防己毒素(一种GABA拮抗剂)非常相似。因此,对方向敏感型神经节细胞的感受野特性进行了详细分析,以研究毒扁豆碱和印防己毒素的作用。

  2. 毒扁豆碱并未消除大小特异性和径向光栅抑制,但它们常受印防己毒素影响。在偏好方向上的最佳速度(通过最大放电频率测量)受毒扁豆碱影响不大,但在注入印防己毒素期间更高。注入烟碱,一种使视网膜神经节细胞活性增加的去极化乙酰胆碱激动剂,揭示了在零方向存在对运动的抑制。印防己毒素注入期间的零方向反应比这种抑制稍晚开始。毒扁豆碱注入期间的零方向反应较弱且开始得更晚。美加明和二氢-β-刺桐啶,烟碱型受体拮抗剂,完全阻断了毒扁豆碱的作用,并使对照光反应降低约一半。

  3. 从该分析来看,开-关型乙酰胆碱释放到方向敏感型细胞上提供了大量兴奋,当被毒扁豆碱增强时,在感受野内克服或超过了零方向的GABA抑制。GABA抑制的空间范围与乙酰胆碱兴奋的空间范围不对称且更大。类似的通路似乎参与了中心-开和开-关方向敏感型神经节细胞,然而中心-开细胞通路可能接受额外输入,该输入在光熄灭时抑制乙酰胆碱兴奋。根据这些结果以及最近的解剖学和药理学发现,讨论了方向敏感性细胞机制的可能方案。

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