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在视网膜切片标本中记录到小鼠双极细胞的两种钙电流。

Two types of calcium currents of the mouse bipolar cells recorded in the retinal slice preparation.

作者信息

de la Villa P, Vaquero C F, Kaneko A

机构信息

Department of Physiology, University of Alcalá de Henares, Madrid, Spain.

出版信息

Eur J Neurosci. 1998 Jan;10(1):317-23. doi: 10.1046/j.1460-9568.1998.00051.x.

Abstract

In the vertebrate retina, the bipolar cell makes reciprocal synapses with amacrine cells at the axon terminal. It has been postulated that amacrine cells may control the transmitter release from bipolar cells by modulating their calcium currents (ICa). To clarify this possibility calcium currents were studied in bipolar cells of the mouse retina using a slice preparation. ICa was identified by voltage clamp protocols, ionic substitution and pharmacological tools. Depolarization to -30 mV from a holding voltage of -80 mV induced an inward current consisting of an initial transient and a long-lasting sustained component. The transient component was inactivated by holding the membrane at more positive voltages. Addition of 100 microM nifedipine suppressed the sustained component, leaving the transient component almost intact. The sustained component was enhanced when external solution contained 0.1 microM Bay K 8644 or when the external Ca2+ was substituted by equimolar Ba2+. Omega-conotoxin (10 microM omega-ctxn GVIA) did not alter either component. We concluded that the transient component is a low-voltage activated T-type ICa, while the sustained component is a high-voltage activated L-type ICa. T-type ICa was recorded in all cells tested, while L-type ICa was found only in cells that retained axon terminals ramifying in the inner plexiform layer. Thus, it is highly likely that L-type ICa is generated at the axon terminal and contributes to the transmitter release from the bipolar cell. The present results confirm that in addition to the T-type ICa that had been previously described, bipolar cells of the mammalian retina also contain L-type ICa similar to the one that has been reported in bipolar cells of the goldfish. The use of retinal slice preparation allowed us to record this current that was not seen previously in the dissociated mouse bipolar cells.

摘要

在脊椎动物视网膜中,双极细胞在轴突末端与无长突细胞形成相互突触。据推测,无长突细胞可能通过调节双极细胞的钙电流(ICa)来控制其递质释放。为了阐明这种可能性,我们使用脑片标本对小鼠视网膜双极细胞的钙电流进行了研究。通过电压钳制方案、离子置换和药理学工具来识别ICa。从-80 mV的钳制电压去极化到-30 mV可诱导出一种内向电流,该电流由一个初始瞬态成分和一个持久的持续成分组成。瞬态成分可通过将膜保持在更正的电压下而失活。加入100 μM硝苯地平可抑制持续成分,而瞬态成分几乎不受影响。当外部溶液含有0.1 μM Bay K 8644或外部Ca2+被等摩尔的Ba2+替代时,持续成分增强。ω-芋螺毒素(10 μM ω-ctxn GVIA)对两种成分均无影响。我们得出结论,瞬态成分是低电压激活的T型ICa,而持续成分是高电压激活的L型ICa。在所测试的所有细胞中均记录到了T型ICa,而仅在那些保留在内网状层中分支的轴突末端的细胞中发现了L型ICa。因此,很可能L型ICa是在轴突末端产生的,并有助于双极细胞释放递质。目前的结果证实,除了先前描述的T型ICa外,哺乳动物视网膜的双极细胞还含有与金鱼双极细胞中报道的类似的L型ICa。使用视网膜脑片标本使我们能够记录到这种以前在解离的小鼠双极细胞中未见的电流。

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