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Tailoring light delivery for optogenetics by modal demultiplexing in tapered optical fibers

机译:通过锥形光纤中的模态解复用来调整光传输以进行光遗传学调整。

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摘要

Optogenetic control of neural activity in deep brain regions ideally requires precise and flexible light delivery with non-invasive devices. To this end, Tapered Optical Fibers (TFs) represent a versatile tool that can deliver light over either large brain volumes or spatially confined sub-regions, while being sensibly smaller than flat-cleaved optical fibers. In this work, we report on the possibility of further extending light emission length along the taper in the range 0.4 mm-3.0 mm by increasing the numerical aperture of the TFs to NA = 0.66. We investigated the dependence between the input angle of light (θin) and the output position along the taper, finding that for θin > 10° this relationship is linear. This mode-division demultiplexing property of the taper was confirmed with a ray tracing model and characterized for 473 nm and 561 nm light in quasi-transparent solution and in brain slices, with the two wavelengths used to illuminate simultaneously two different regions of the brain using only one waveguide. The results presented in this manuscript can guide neuroscientists to design their optogenetic experiments on the base of this mode-division demultiplexing approach, providing a tool that potentially allow for dynamic targeting of regions with diverse extension, from the mouse VTA up to the macaque visual cortex.
机译:理想的是,对大脑深部区域的神经活动进行光遗传学控制需要使用非侵入性设备进行精确而灵活的光传输。为此,锥形光纤(TFs)代表了一种多功能的工具,它可以在较大的大脑体积或空间受限的子区域上传递光,同时比扁平切割的光纤更小。在这项工作中,我们报告了通过将TF的数值孔径增加到NA = 0.66来进一步在0.4 mm-3.0 mm范围内沿锥度扩展发光长度的可能性。我们研究了光的输入角度(θin)与沿锥度的输出位置之间的相关性,发现对于θin> 10°,此关系是线性的。锥度的这种模式划分多路分解特性已通过射线追踪模型得到了证实,并针对准透明溶液和脑切片中的473 nm和561 nm的光进行了表征,这两个波长用于同时照亮大脑的两个不同区域只有一个波导。本手稿中的结果可以指导神经科学家在这种模式分割多路分解方法的基础上设计光遗传学实验,提供一种工具,可以动态定位从鼠标VTA到猕猴视觉皮层等具有多种延伸范围的区域。 。

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