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小鼠视锥光感受器中存在功能性GABAA受体而非GABAC受体的证据。

Evidence for functional GABAA but not GABAC receptors in mouse cone photoreceptors.

作者信息

Deniz Sercan, Wersinger Eric, Picaud Serge, Roux Michel J

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, Department of Translational Medicine and Neurogenetics, F-67404, Illkirch, France.

Centre National de la Recherche Scientifique, UMR7104, F-67404, Illkirch, France.

出版信息

Vis Neurosci. 2019 Jan;36:E005. doi: 10.1017/S0952523819000038.

Abstract

At the first retinal synapse, horizontal cells (HCs) contact both photoreceptor terminals and bipolar cell dendrites, modulating information transfer between these two cell types to enhance spatial contrast and mediate color opponency. The synaptic mechanisms through which these modulations occur are still debated. The initial hypothesis of a GABAergic feedback from HCs to cones has been challenged by pharmacological inconsistencies. Surround antagonism has been demonstrated to occur via a modulation of cone calcium channels through ephaptic signaling and pH changes in the synaptic cleft. GABAergic transmission between HCs and cones has been reported in some lower vertebrates, like the turtle and tiger salamander. In these reports, it was revealed that GABA is released from HCs through reverse transport and target GABA receptors are located at the cone terminals. In mammalian retinas, there is growing evidence that HCs can release GABA through conventional vesicular transmission, acting both on autaptic GABA receptors and on receptors expressed at the dendritic tips of the bipolar cells. The presence of GABA receptors on mammalian cone terminals remains equivocal. Here, we looked specifically for functional GABA receptors in mouse photoreceptors by recording in the whole-cell or amphotericin/gramicidin-perforated patch clamp configurations. Cones could be differentiated from rods through morphological criteria. Local GABA applications evoked a Cl- current in cones but not in rods. It was blocked by the GABAA receptor antagonist bicuculline methiodide and unaffected by the GABAC receptor antagonist TPMPA [(1,2,5,6-tetrahydropyridin-4-yl)methylphosphinic acid]. The voltage dependency of the current amplitude was as expected from a direct action of GABA on cone pedicles but not from an indirect modulation of cone currents following the activation of the GABA receptors of HCs. This supports a direct role of GABA released from HCs in the control of cone activity in the mouse retina.

摘要

在视网膜的第一个突触处,水平细胞(HCs)与光感受器终端和双极细胞树突均有接触,调节这两种细胞类型之间的信息传递,以增强空间对比度并介导颜色拮抗。这些调节作用发生的突触机制仍存在争议。最初关于HCs向视锥细胞进行GABA能反馈的假说已受到药理学不一致性的挑战。已证明周围拮抗作用是通过电突触信号传导和突触间隙pH变化对视锥细胞钙通道的调节而发生的。在一些低等脊椎动物,如乌龟和虎螈中,已报道了HCs与视锥细胞之间的GABA能传递。在这些报道中,发现GABA通过逆向转运从HCs释放,且靶GABA受体位于视锥细胞终端。在哺乳动物视网膜中,越来越多的证据表明HCs可通过传统的囊泡传递释放GABA,其作用于自身突触GABA受体以及双极细胞树突尖端表达的受体。哺乳动物视锥细胞终端上GABA受体的存在仍不明确。在此,我们通过全细胞或两性霉素/短杆菌肽穿孔膜片钳记录方式,专门在小鼠光感受器中寻找功能性GABA受体。视锥细胞可通过形态学标准与视杆细胞区分开来。局部应用GABA可在视锥细胞中诱发Cl-电流,但在视杆细胞中则无此现象。该电流被GABAA受体拮抗剂甲基荷包牡丹碱阻断,且不受GABAC受体拮抗剂TPMPA [(1,2,5,6-四氢吡啶-4-基)甲基次膦酸]的影响。电流幅度的电压依赖性符合GABA对视锥细胞蒂的直接作用预期,而非HCs的GABA受体激活后视锥细胞电流的间接调节。这支持了HCs释放的GABA在控制小鼠视网膜视锥细胞活性中具有直接作用。

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