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合成视网膜类似物可改变微生物视紫红质光遗传学工具的光谱和动力学特性。

Synthetic retinal analogues modify the spectral and kinetic characteristics of microbial rhodopsin optogenetic tools.

机构信息

1] Buchmann Institute for Molecular Life Sciences (BMLS), Goethe-University, Max-von-Laue-Straße 15, 60438 Frankfurt, Germany [2] Institute of Biochemistry, Goethe-University, Max-von-Laue-Straße 9, 60438 Frankfurt, Germany.

Institute for Biology-Experimental Biophysics, Humboldt-Universität zu Berlin, Invalidenstraße 42, 10115 Berlin, Germany.

出版信息

Nat Commun. 2014 Dec 15;5:5810. doi: 10.1038/ncomms6810.

Abstract

Optogenetic tools have become indispensable in neuroscience to stimulate or inhibit excitable cells by light. Channelrhodopsin-2 (ChR2) variants have been established by mutating the opsin backbone or by mining related algal genomes. As an alternative strategy, we surveyed synthetic retinal analogues combined with microbial rhodopsins for functional and spectral properties, capitalizing on assays in C. elegans, HEK cells and larval Drosophila. Compared with all-trans retinal (ATR), Dimethylamino-retinal (DMAR) shifts the action spectra maxima of ChR2 variants H134R and H134R/T159C from 480 to 520 nm. Moreover, DMAR decelerates the photocycle of ChR2(H134R) and (H134R/T159C), thereby reducing the light intensity required for persistent channel activation. In hyperpolarizing archaerhodopsin-3 and Mac, naphthyl-retinal and thiophene-retinal support activity alike ATR, yet at altered peak wavelengths. Our experiments enable applications of retinal analogues in colour tuning and altering photocycle characteristics of optogenetic tools, thereby increasing the operational light sensitivity of existing cell lines or transgenic animals.

摘要

光遗传学工具已经成为神经科学中不可或缺的手段,可通过光来刺激或抑制可兴奋细胞。通过突变视蛋白骨干或挖掘相关藻类基因组,已经建立了通道视紫红质-2(ChR2)变体。作为一种替代策略,我们调查了与微生物视蛋白相结合的合成视网膜类似物的功能和光谱特性,利用秀丽隐杆线虫、HEK 细胞和幼虫果蝇中的测定方法。与全反式视黄醛(ATR)相比,二甲基氨基视黄醛(DMAR)将 ChR2 变体 H134R 和 H134R/T159C 的作用光谱最大值从 480nm 移动到 520nm。此外,DMAR 减缓了 ChR2(H134R)和(H134R/T159C)的光循环,从而减少了持续通道激活所需的光强度。在超极化古菌视紫红质-3 和 Mac 中,萘基视黄醛和噻吩视黄醛支持与 ATR 类似的活性,但在改变的峰值波长下。我们的实验使视网膜类似物能够应用于颜色调谐和改变光遗传学工具的光循环特性,从而提高现有细胞系或转基因动物的操作光敏感性。

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