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虎螈视网膜双极细胞的感受野:一项药理学研究

Receptive field of the retinal bipolar cell: a pharmacological study in the tiger salamander.

作者信息

Hare W A, Owen W G

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley 94720, USA.

出版信息

J Neurophysiol. 1996 Sep;76(3):2005-19. doi: 10.1152/jn.1996.76.3.2005.

Abstract
  1. It is widely believed that signals contributing to the receptive field surrounds of retinal bipolar cells pass from horizontal cells to bipolar cells via GABAergic synapses. To test this notion, we applied gamma-aminobutyric acid (GABA) agonists and antagonists to isolated, perfused retinas of the salamander Ambystoma tigrinum while recording intracellularly from bipolar cells, horizontal cells, and photoreceptors. 2. As we previously reported, administration of the GABA analogue D-aminovaleric acid in concert with picrotoxin did not block horizontal cell responses or the center responses of bipolar cells but blocked the surround responses of both on-center and off-center bipolar cells. 3. Surround responses were not blocked by the GABA, antagonists picrotoxin or bicuculline, the GABAB agonist baclofen or the GABAB antagonist phaclofen, and the GABAC antagonists picrotoxin or cis-4-aminocrotonic acid. Combinations of these drugs were similarly ineffective. 4. GABA itself activated a powerful GABA uptake mechanism in horizontal cells for which nipecotic acid is a competitive agonist. It also activated, both in horizontal cells and bipolar cells, large GABAA conductances that shunted light responses but that could be blocked by picrotoxin or bicuculline. 5. GABA, administered together with picrotoxin to block the shunting effect of GABAA activation, did not eliminate bipolar cell surround responses at concentrations sufficient to saturate the known types of GABA receptors. 6. Surround responses were not blocked by glycine or its antagonist strychnine, or by combinations of drugs designed to eliminate GABAergic and glycinergic pathways simultaneously. 7. Although we cannot fully discount the involvement of a novel GABAergic synapse, the simplest explanation of our findings is that the primary pathway mediating the bipolar cell's surround is neither GABAergic nor glycinergic.
摘要
  1. 人们普遍认为,构成视网膜双极细胞感受野周边的信号是通过γ-氨基丁酸(GABA)能突触从水平细胞传递到双极细胞的。为了验证这一观点,我们将γ-氨基丁酸(GABA)激动剂和拮抗剂应用于分离并灌注的虎纹钝口螈视网膜,同时从双极细胞、水平细胞和光感受器进行细胞内记录。2. 正如我们之前所报道的,将GABA类似物D-氨基戊酸与苦味毒一起施用,并未阻断水平细胞反应或双极细胞的中心反应,但阻断了on-center和off-center双极细胞的周边反应。3. 周边反应不受GABA拮抗剂苦味毒或荷包牡丹碱、GABAB激动剂巴氯芬或GABAB拮抗剂法氯芬以及GABAC拮抗剂苦味毒或顺式-4-氨基巴豆酸的阻断。这些药物的组合同样无效。4. GABA本身在水平细胞中激活了一种强大的GABA摄取机制,烟碱酸是其竞争性激动剂。它还在水平细胞和双极细胞中激活了大的GABAA电导,这些电导会分流光反应,但可被苦味毒或荷包牡丹碱阻断。5. 将GABA与苦味毒一起施用以阻断GABAA激活的分流效应,在足以使已知类型的GABA受体饱和的浓度下,并未消除双极细胞的周边反应。6. 周边反应不受甘氨酸或其拮抗剂士的宁的阻断,也不受旨在同时消除GABA能和甘氨酸能途径的药物组合的阻断。7. 尽管我们不能完全排除新型GABA能突触的参与,但对我们研究结果最简单的解释是,介导双极细胞周边反应的主要途径既不是GABA能的也不是甘氨酸能的。

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