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In Situ Real-Time Monitoring of Glutamate and Electrophysiology from Cortex to Hippocampus in Mice Based on a Microelectrode Array

机译:基于微电极阵列的小鼠皮质至海马谷氨酸和电生理的原位实时监测

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Changes in the structure and function of the hippocampus contribute to epilepsy, schizophrenia and other neurological or mental disorders of the brain. Since the function of the hippocampus depends heavily on the glutamate (Glu) signaling pathways, in situ real-time detection of Glu neurotransmitter release and electrophysiological signals in hippocampus is of great significance. To achieve the dual-mode detection in mouse hippocampus in vivo, a 16-channel implantable microelectrode array (MEA) was fabricated by micro-electromechanical system (MEMS) technology. Twelve microelectrode sites were modified with platinum black for electrophysiological recording and four sites were modified with glutamate oxidase (GluOx) and 1,3-phenylenediamine (mPD) for selective electrochemical detection of Glu. The MEA was implanted from cortex to hippocampus in mouse brain for in situ real-time monitoring of Glu and electrophysiological signals. It was found that the Glu concentration in hippocampus was roughly 50 μM higher than that in the cortex, and the firing rate of concurrently recorded spikes declined from 6.32 ± 4.35 spikes/s in cortex to 0.09 ± 0.06 spikes/s in hippocampus. The present results demonstrated that the dual-mode MEA probe was capable in neurological detections in vivo with high spatial resolution and dynamical response, which lays the foundation for further pathology studies in the hippocampus of mouse models with nervous or mental disorders.
机译:海马结构和功能的变化会导致癫痫,精神分裂症和其他大脑神经或精神疾病。由于海马的功能在很大程度上依赖于谷氨酸(Glu)信号通路,因此就地实时检测海马中Glu神经递质的释放和电生理信号具有重要意义。为了在小鼠海马体内实现双模式检测,通过微机电系统(MEMS)技术制备了16通道可植入微电极阵列(MEA)。用铂黑修饰了12个微电极位点以进行电生理记录,并用谷氨酸氧化酶(GluOx)和1,3-苯二胺(mPD)修饰了4个位点以选择性地电化学检测Glu。 MEA被植入小鼠大脑皮层至海马体中,以实时监测Glu和电生理信号。发现海马中的Glu浓度比皮层中的Glu浓度高约50μM,同时记录的尖峰发射速率从皮层中的6.32±4.35尖峰/秒降低到海马中的0.09±0.06尖峰/秒。目前的结果表明,双模式MEA探针能够在体内以高空间分辨率和动态响应进行神经学检测,从而为神经或精神疾病小鼠模型的海马进一步病理研究奠定了基础。

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