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Readily evoked forelimb movement in rat via optogenetic stimulation of motor cortex

机译:通过运动皮层的光遗传学刺激诱发大鼠前肢运动

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Virally transfected optogenetics is emerging as a powerful tool for studying neural circuits and behavior in non-genetically tractable animals. A basic test of this tool is the ability to evoke movement by cortical stimulation. While evoked movements have been reported in transgenic mice, there is concern that optogenetic stimulation has not readily evoked skeletal movements in rat or monkey. Here we show that optogenetics can drive limb movements in rat. We injected AAV vectors with channelrhodopsin-2 into deep layers of rat primary motor cortex (M1). Subsequent optical stimulation of M1 elicted robust limb movements in anesthetized animals; anesthesia rules out the possibility that movement is an indirect behavioral response to the stimulation. Histology shows expression in corticospinal neurons, and movement may have been mediated by direct activation of these cells. Our results suggest two factors that may be critical for optogenetically evoking movements in virally transfected animals: a sparse (< 5%) pattern of distribution of transfected neurons, including corticospinal neurons, and a high power density of stimulation (>1200 mW/mm2) in the deep layers (at least 1.1 mm below cortical surface).
机译:病毒转染的光遗传学正在成为研究非遗传易处理动物的神经回路和行为的有力工具。该工具的基本测试是通过皮层刺激引起运动的能力。虽然在转基因小鼠中已经报道了诱发运动,但是人们担心光遗传学刺激不能轻易诱发大鼠或猴子的骨骼运动。在这里,我们证明了光遗传学可以驱动大鼠肢体运动。我们将带有通道视紫红质2的AAV载体注入大鼠原代运动皮层(M1)的深层。随后对M1的光刺激在麻醉动物中引起了强烈的肢体运动。麻醉排除了运动是对刺激的间接行为反应的可能性。组织学显示在皮质脊髓神经元中表达,并且运动可能已经由这些细胞的直接激活介导。我们的结果表明,对于病毒转染的动物的光遗传诱发运动可能至关重要的两个因素:转染的神经元(包括皮质脊髓神经元)分布的稀疏(<5%)模式和高功率刺激密度(> 1200 mW / mm2)在深层(皮层表面以下至少1.1毫米)。

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