Nitric oxide modulates contrast suppression in a subset of mouse retinal ganglion cells

神经科学 视网膜 视网膜 感受野 视网膜神经节细胞 生物 神经调节 明视 电池类型 对比度(视觉) 巨大视网膜神经节细胞 生物神经网络 视网膜波 中枢神经系统 细胞 物理 光学 生物化学 遗传学
作者
Dominic Gonschorek,Matías A. Goldin,Jonathan Oesterle,Tom Schwerd-Kleine,Ryan Arlinghaus,Zhijian Zhao,Timm Schubert,Olivier Marre,Thomas Euler
标识
DOI:10.7554/elife.98742
摘要

Neuromodulators have major influences on the regulation of neural circuit activity across the nervous system. Nitric oxide (NO) has been shown to be a prominent neuromodulator in many circuits and has been extensively studied in the retina. Here, it has been associated with the regulation of light adaptation, gain control, and gap junctional coupling, but its effect on the retinal output, specifically on the different types of retinal ganglion cells (RGCs), is still poorly understood. In this study, we used two-photon Ca 2+ imaging and multi-electrode array (MEA) recordings to measure light-evoked activity of RGCs in the ganglion cell layer in the ex vivo mouse retina. This approach allowed us to investigate the neuromodulatory effects of NO on a cell type-level. Our findings reveal that NO selectively modulates the suppression of temporal responses in a distinct subset of contrast-suppressed RGC types, increasing their activity without altering the spatial properties of their receptive fields. Given that NO release is triggered by quick changes in light levels under photopic conditions, we propose that these RGC types signal fast contrast changes to higher visual regions. Remarkably, we found that about one-third of the RGC types, recorded using two-photon Ca 2+ imaging, exhibited consistent, cell type-specific adaptational response changes throughout an experiment, independent of NO. By employing a paired-recording paradigm, we could disentangle those additional adaptational response changes from drug-induced modulations. Taken together, our research highlights the selective neuromodulatory effects of NO on RGCs and emphasizes the need of considering non-pharmacological activity changes, like adaptation, in such study designs.

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