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通过仿生化学神经调节恢复视力的外源性谷氨酸的视网膜下注射深度研究。

Investigation of Injection Depth for Subretinal Delivery of Exogenous Glutamate to Restore Vision via Biomimetic Chemical Neuromodulation.

出版信息

IEEE Trans Biomed Eng. 2020 Feb;67(2):464-470. doi: 10.1109/TBME.2019.2915255. Epub 2019 May 7.

Abstract

Chemical neuromodulation of the retina using native neurotransmitters to biomimetically activate target retinal neurons through chemical synapses is a promising biomimetic alternative to electrical stimulation for restoring vision in blindness caused by photoreceptor degenerative diseases. Recent research has shown that subretinal chemical stimulation could be advantageous for treating photoreceptor degenerative diseases but many of the parameters for achieving efficacious chemical neuromodulation are yet to be explored. In this paper, we investigated how the depth at which neurotransmitter is injected subretinally affects the success rate, spike rate characteristics (i.e., amplitude, response latency, and time width), and spatial resolution of chemical stimulation in wild-type Long Evans and photoreceptor degenerated S334ter-3 transgenic rat retinas in vitro. We compared the responses to injections of glutamate at the subretinal surface and two subsurface depths near the outer and inner plexiform layers and found that while injections at all depths elicited robust retinal ganglion cell responses, they differed significantly in terms of the spike rate characteristics and spatial resolutions across injection depths. Shallow subsurface injections near the outer plexiform layer evoked the highest spike rate amplitudes and had the highest spatial resolution and success rates, while deep subsurface injections near the inner plexiform layer elicited the shortest latencies and narrowest time widths. Our results suggest that surface injections are suboptimal for subretinal chemical neuromodulation, while shallow subsurface and deep subsurface injections may optimize high spatial and high temporal resolution, respectively. These findings have great significance for the design and development of a potential neurotransmitter-based subretinal prosthesis.

摘要

使用内源性神经递质对视网膜进行化学神经调节,通过化学突触仿生激活靶向视网膜神经元,这是一种有前途的仿生替代方法,可替代电刺激,用于治疗由光感受器退行性疾病引起的失明。最近的研究表明,视网膜下化学刺激可能有利于治疗光感受器退行性疾病,但仍有许多实现有效化学神经调节的参数有待探索。在本文中,我们研究了神经递质在视网膜下注射的深度如何影响成功率、尖峰率特征(即幅度、响应潜伏期和时间宽度)以及野生型 Long Evans 和光感受器退行性 S334ter-3 转基因大鼠视网膜体外化学刺激的空间分辨率。我们比较了在视网膜下表面和靠近外丛状层和内丛状层的两个亚表面深度注射谷氨酸的反应,发现虽然所有深度的注射都引起了强烈的视网膜神经节细胞反应,但它们在尖峰率特征和空间分辨率方面存在显著差异。靠近外丛状层的浅层亚表面注射引起的尖峰率幅度最高,空间分辨率和成功率最高,而靠近内丛状层的深层亚表面注射引起的潜伏期最短,时间宽度最窄。我们的结果表明,表面注射对于视网膜下化学神经调节来说不是最佳选择,而浅层亚表面和深层亚表面注射可能分别优化了高空间分辨率和高时间分辨率。这些发现对于基于神经递质的潜在视网膜下假体的设计和开发具有重要意义。

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