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表达两种不同类型通道视紫红质基因的光感受器变性大鼠的视觉反应。

Visual Responses of Photoreceptor-Degenerated Rats Expressing Two Different Types of Channelrhodopsin Genes.

机构信息

Laboratory of Visual Neuroscience, Graduate Course in Biological Sciences, Iwate University Division of Science and Engineering, 4-3-5 Ueda, Morioka, Iwate 020-8551, Japan.

Soft-Path Engineering Research Center (SPERC), Iwate University Division of Science and Engineering, Morioka 020-8551, Japan.

出版信息

Sci Rep. 2017 Jan 23;7:41210. doi: 10.1038/srep41210.

Abstract

Optogenetic technologies are expected to be applicable for clinical use in restoring vision. However, the degree of recovered visual function is highly dependent on the function of the chosen optogenetic gene. To investigate the effect on visual function of dual expression of genes with different wavelength sensitivities, we transduced a modified Volvox-derived channelrhodopsin gene (mVChR1) via an adeno-associated virus vector into transgenic rats harbouring the ChR2 gene in retinal ganglion cells. These transgenic rats were given an intraperitoneal injection of N-methyl-N-nitrosourea to induce the degeneration of native photoreceptor cells prior to transduction of mVChR1. Optical coherence tomography images indicated the degeneration of the native photoreceptor cells after the N-methyl-N-nitrosourea injection. Complete loss of function of the native photoreceptor cells was confirmed using electroretinograms. In the ChR2 transgenic rats, visually evoked potentials were clearly detectable in spite of native photoreceptor function abolishment; however the responses were limited to within blue wavelengths. In contrast, the limited wavelength sensitivities were improved by the additional transduction of mVChR1, which exhibited sensitivities to green and red. Thus, the transductions of dual genes encoding channelrhodopsins that exhibit different wavelength sensitivities represents a promising candidate method to expand and to enhance rescued wavelength sensitivities in blind subjects.

摘要

光遗传学技术有望应用于恢复视力的临床治疗。然而,恢复的视觉功能的程度高度依赖于所选择的光遗传学基因的功能。为了研究不同波长敏感性的双基因表达对视觉功能的影响,我们通过腺相关病毒载体将改良的 Volvox 衍生的通道视紫红质基因 (mVChR1) 转导到视网膜神经节细胞中携带 ChR2 基因的转基因大鼠中。这些转基因大鼠在转导 mVChR1 之前通过腹腔注射 N-甲基-N-亚硝脲诱导内源性光感受器细胞变性。光学相干断层扫描图像表明 N-甲基-N-亚硝脲注射后内源性光感受器细胞的变性。使用视网膜电图证实了内源性光感受器细胞的完全失活功能。在 ChR2 转基因大鼠中,尽管内源性光感受器功能丧失,但视觉诱发电位仍可清晰检测到;然而,反应仅限于蓝色波长范围内。相比之下,通过额外转导 mVChR1 改善了有限的波长敏感性,mVChR1 对绿光和红光敏感。因此,转导编码具有不同波长敏感性的双基因的通道视紫红质代表了一种有前途的候选方法,可以扩大和增强盲人群体中获救的波长敏感性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/740b/5255552/9a1cbd7e4bac/srep41210-f1.jpg

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