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T-DOpE 探针揭示了行为小鼠中海马体振荡对大麻素的敏感性。

T-DOpE probes reveal sensitivity of hippocampal oscillations to cannabinoids in behaving mice.

机构信息

The Bradley Department of Electrical and Computer Engineering, Virginia Tech, Blacksburg, VA, USA.

School of Neuroscience, Virginia Tech, Blacksburg, VA, USA.

出版信息

Nat Commun. 2024 Feb 24;15(1):1686. doi: 10.1038/s41467-024-46021-4.

Abstract

Understanding the neural basis of behavior requires monitoring and manipulating combinations of physiological elements and their interactions in behaving animals. We developed a thermal tapering process enabling fabrication of low-cost, flexible probes combining ultrafine features: dense electrodes, optical waveguides, and microfluidic channels. Furthermore, we developed a semi-automated backend connection allowing scalable assembly. We demonstrate T-DOpE (Tapered Drug delivery, Optical stimulation, and Electrophysiology) probes achieve in single neuron-scale devices (1) high-fidelity electrophysiological recording (2) focal drug delivery and (3) optical stimulation. The device tip can be miniaturized (as small as 50 µm) to minimize tissue damage while the ~20 times larger backend allows for industrial-scale connectorization. T-DOpE probes implanted in mouse hippocampus revealed canonical neuronal activity at the level of local field potentials (LFP) and neural spiking. Taking advantage of the triple-functionality of these probes, we monitored LFP while manipulating cannabinoid receptors (CB1R; microfluidic agonist delivery) and CA1 neuronal activity (optogenetics). Focal infusion of CB1R agonist downregulated theta and sharp wave-ripple oscillations (SPW-Rs). Furthermore, we found that CB1R activation reduces sharp wave-ripples by impairing the innate SPW-R-generating ability of the CA1 circuit.

摘要

理解行为的神经基础需要监测和操纵行为动物中生理元素及其相互作用的组合。我们开发了一种热缩过程,能够制造出低成本、灵活的探针,结合超细特征:密集的电极、光学波导和微流道。此外,我们开发了一种半自动后端连接,允许可扩展的组装。我们展示了 T-DOpE(锥形药物输送、光学刺激和电生理学)探针在单个神经元尺度的设备中实现了 (1) 高保真电生理记录,(2) 焦点药物输送和 (3) 光学刺激。器件尖端可以微型化(小至 50µm),以最小化组织损伤,而大约 20 倍更大的后端允许工业规模的连接器化。植入小鼠海马体的 T-DOpE 探针揭示了局部场电位 (LFP) 和神经尖峰水平的典型神经元活动。利用这些探针的三重功能,我们在操纵大麻素受体 (CB1R;微流控激动剂输送) 和 CA1 神经元活动 (光遗传学) 的同时监测 LFP。CB1R 激动剂的焦点输注下调了θ波和锐波-涟漪振荡 (SPW-Rs)。此外,我们发现 CB1R 激活通过损害 CA1 电路产生固有 SPW-R 的能力来减少锐波涟漪。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dbd9/10894268/436e72f2116e/41467_2024_46021_Fig1_HTML.jpg

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