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In vivo monitoring of glial scar proliferation on chronically implanted neural electrodes by fiber optical coherence tomography

机译:光纤相干断层扫描在体内监测慢性植入神经电极上的神经胶质瘢痕增生

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摘要

In neural prosthetics and stereotactic neurosurgery, intracortical electrodes are often utilized for delivering therapeutic electrical pulses, and recording neural electrophysiological signals. Unfortunately, neuroinflammation impairs the neuron-electrode-interface by developing a compact glial encapsulation around the implants in long term. At present, analyzing this immune reaction is only feasible with post-mortem histology; currently no means for specific in vivo monitoring exist and most applicable imaging modalities can not provide information in deep brain regions. Optical coherence tomography (OCT) is a well established imaging modality for in vivo studies, providing cellular resolution and up to 1.2 mm imaging depth in brain tissue. A fiber based spectral domain OCT was shown to be capable of minimally invasive brain imaging. In the present study, we propose to use a fiber based spectral domain OCT to monitor the progression of the tissue's immune response through scar encapsulation progress in a rat animal model. A fine fiber catheter was implanted in rat brain together with a flexible polyimide microelectrode in sight both of which acts as a foreign body and induces the brain tissue immune reaction. OCT signals were collected from animals up to 12 weeks after implantation and thus gliotic scarring in vivo monitored for that time. Preliminary data showed a significant enhancement of the OCT backscattering signal during the first 3 weeks after implantation, and increased attenuation factor of the sampled tissue due to the glial scar formation.
机译:在神经修复术和立体定向神经外科手术中,皮质内电极通常用于传递治疗性电脉冲和记录神经电生理信号。不幸的是,神经炎症会通过长期在植入物周围形成紧密的神经胶质包囊而损害神经元-电极界面。目前,仅在验尸组织学中分析这种免疫反应是可行的。目前尚无用于特定体内监测的方法,并且大多数适用的成像方式无法在大脑深部区域提供信息。光学相干断层扫描(OCT)是一种用于体内研究的成熟成像方式,可提供脑组织的细胞分辨率和高达1.2 mm的成像深度。基于纤维的光谱域OCT被证明能够进行微创脑成像。在本研究中,我们建议使用基于纤维的光谱域OCT来通过大鼠动物模型中的瘢痕包封进展监测组织免疫应答的进展。将细纤维导管与可见的柔性聚酰亚胺微电极一起植入大鼠脑中,两者均充当异物并诱导脑组织免疫反应。植入后最多12周从动物收集OCT信号,因此在这段时间内可以监测体内的神经胶质瘢痕形成。初步数据显示,在植入后的最初3周内,OCT背向散射信号显着增强,并且由于神经胶质瘢痕的形成,导致采样组织的衰减因子增加。

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