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ON通路阻断对兔视网膜方向选择性的影响。

Effect of ON pathway blockade on directional selectivity in the rabbit retina.

作者信息

Kittila C A, Massey S C

机构信息

Sensory Sciences Center, University of Texas Health Science Center, Graduate School of Biomedical Sciences, Houston 77030, USA.

出版信息

J Neurophysiol. 1995 Feb;73(2):703-12. doi: 10.1152/jn.1995.73.2.703.

Abstract
  1. In this report we describe extracellular recordings made from directionally selective (DS) ganglion cells in the rabbit retina during perfusion with 2-amino-4-phosphonobutyric acid (APB) to block ON channels through the retina. 2. Application of 100 microM APB selectively and reversibly abolished the responses of ON ganglion cells in the rabbit retina. In addition, 100 microM APB completely and reversibly blocked ON component responses of ON-OFF DS ganglion cells to both stationary and moving stimuli. These results are consistent with the idea that APB blocks ON pathways through the retina. 3. Under ON pathway blockade with APB, OFF component responses of ON-OFF DS ganglion cells remained DS. DS OFF responses retained the same preferred direction as the pre-APB ON-OFF responses and could be driven using either normal or reversed contrast stimuli. 4. Extracellular responses of ON DS ganglion cells were completely blocked by APB. Under APB, these cells showed no response to stationary or moving stimuli. 5. Application of the gamma-aminobutyric acid-A (GABAA) antagonist 2-(3-Carboxypropyl)-3-amino-6-(4-methoxyphenyl)pyridazinium bromide (SR95531) reversibly abolished directional selectivity of ON DS and ON-OFF DS ganglion cells in the rabbit retina. This finding is consistent with previous data for picrotoxin. 6. Application of SR95531 during ON channel blockade by APB caused OFF component responses of ON-OFF DS ganglion cells to lose their directional selectivity. Under these conditions, OFF responses to movement in the preferred and null directions became virtually identical. 7. These results indicate that simultaneous ON and OFF layer input is not required to generate directional responses in ON-OFF DS ganglion cells. In addition, it appears that a GABAA-dependent mechanism for directional selectivity may operate independently in the two separate dendritic layers of the ON-OFF DS ganglion cell.
摘要
  1. 在本报告中,我们描述了在灌注2-氨基-4-膦酰丁酸(APB)以阻断整个视网膜上的ON通道期间,从兔视网膜中方向选择性(DS)神经节细胞进行的细胞外记录。2. 应用100微摩尔APB选择性且可逆地消除了兔视网膜中ON神经节细胞的反应。此外,100微摩尔APB完全且可逆地阻断了ON-OFF DS神经节细胞对静止和移动刺激的ON成分反应。这些结果与APB阻断通过视网膜的ON通路这一观点一致。3. 在APB阻断ON通路的情况下,ON-OFF DS神经节细胞的OFF成分反应仍保持方向选择性。DS OFF反应保留了与APB处理前ON-OFF反应相同的偏好方向,并且可以使用正常或反转对比度刺激来驱动。4. APB完全阻断了ON DS神经节细胞的细胞外反应。在APB作用下,这些细胞对静止或移动刺激均无反应。5. 应用γ-氨基丁酸-A(GABAA)拮抗剂2-(3-羧丙基)-3-氨基-6-(4-甲氧基苯基)哒嗪溴化物(SR95531)可逆地消除了兔视网膜中ON DS和ON-OFF DS神经节细胞的方向选择性。这一发现与之前关于印防己毒素的数据一致。6. 在APB阻断ON通道期间应用SR95531,导致ON-OFF DS神经节细胞的OFF成分反应失去其方向选择性。在这些条件下,对偏好方向和零方向运动的OFF反应实际上变得相同。7. 这些结果表明,在ON-OFF DS神经节细胞中产生方向反应不需要同时有ON层和OFF层输入。此外,似乎一种依赖GABAA的方向选择性机制可能在ON-OFF DS神经节细胞的两个独立树突层中独立运作。

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