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通过外周神经刺激对中期鸡胚腿部运动进行光遗传调控。

Optogenetic regulation of leg movement in midstage chick embryos through peripheral nerve stimulation.

机构信息

Dept. of Anatomy, Southern Illinois Univ. School of Medicine, 1135 Lincoln Dr., Carbondale, IL 62901-6523, USA.

出版信息

J Neurophysiol. 2011 Nov;106(5):2776-82. doi: 10.1152/jn.00712.2011. Epub 2011 Aug 31.

DOI:10.1152/jn.00712.2011
PMID:21880945
Abstract

Numerous disorders that affect proper development, including the structure and function of the nervous system, are associated with altered embryonic movement. Ongoing challenges are to understand in detail how embryonic movement is generated and to understand better the connection between proper movement and normal nervous system function. Controlled manipulation of embryonic limb movement and neuronal activity to assess short- and long-term outcomes can be difficult. Optogenetics is a powerful new approach to modulate neuronal activity in vivo. In this study, we have used an optogenetics approach to activate peripheral motor axons and thus alter leg motility in the embryonic chick. We used electroporation of a transposon-based expression system to produce ChIEF, a channelrhodopsin-2 variant, in the lumbosacral spinal cord of chick embryos. The transposon-based system allows for stable incorporation of transgenes into the genomic DNA of recipient cells. ChIEF protein is detectable within 24 h of electroporation, largely membrane-localized, and found throughout embryonic development in both central and peripheral processes. The optical clarity of thin embryonic tissue allows detailed innervation patterns of ChIEF-containing motor axons to be visualized in the living embryo in ovo, and pulses of blue light delivered to the thigh can elicit stereotyped flexures of the leg when the embryo is at rest. Continuous illumination can disrupt full extension of the leg during spontaneous movements. Therefore, our results establish an optogenetics approach to alter normal peripheral axon function and to probe the role of movement and neuronal activity in sensorimotor development throughout embryogenesis.

摘要

许多影响正常发育的疾病,包括神经系统的结构和功能,都与胚胎运动的改变有关。目前的挑战是详细了解胚胎运动是如何产生的,并更好地理解正常运动与正常神经系统功能之间的联系。控制胚胎肢体运动和神经元活动以评估短期和长期结果可能很困难。光遗传学是一种调节体内神经元活动的强大新方法。在这项研究中,我们使用光遗传学方法激活周围运动轴突,从而改变鸡胚的腿部运动。我们使用基于转座子的表达系统的电穿孔在鸡胚的腰骶脊髓中产生 ChIEF,一种通道视紫红质-2 变体。基于转座子的系统允许将转基因稳定整合到受体细胞的基因组 DNA 中。ChIEF 蛋白在电穿孔后 24 小时内可检测到,主要定位于细胞膜,并在胚胎发育过程中在中枢和周围过程中均有发现。薄的胚胎组织的光学透明度允许在活体胚胎中观察到含有 ChIEF 的运动轴突的详细神经支配模式,并在胚胎静止时向大腿传递蓝色光脉冲可以引起腿部的刻板屈曲。连续光照会破坏自发运动过程中腿部的完全伸展。因此,我们的结果建立了一种光遗传学方法来改变正常的周围轴突功能,并探究运动和神经元活动在整个胚胎发生过程中的感觉运动发育中的作用。

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