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In vivo Characterization of Amorphous Silicon Carbide As a Biomaterial for Chronic Neural Interfaces

机译:体内表征非晶碳化硅作为慢性神经接口的生物材料

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摘要

Implantable microelectrode arrays (MEAs) offer clinical promise for prosthetic devices by enabling restoration of communication and control of artificial limbs. While proof-of-concept recordings from MEAs have been promising, work in animal models demonstrates that the obtained signals degrade over time. Both material robustness and tissue response are acknowledged to have a role in device lifetime. Amorphous Silicon carbide (a-SiC), a robust material that is corrosion resistant, has emerged as an alternative encapsulation layer for implantable devices. We systematically examined the impact of a-SiC coating on Si probes by immunohistochemical characterization of key markers implicated in tissue-device response. After implantation, we performed device capture immunohistochemical labeling of neurons, astrocytes, and activated microglia/macrophages after 4 and 8 weeks of implantation. Neuron loss and microglia activation were similar between Si and a-SiC coated probes, while tissue implanted with a-SiC displayed a reduction in astrocytes adjacent to the probe. These results suggest that a-SiC has a similar biocompatibility profile as Si, and may be suitable for implantable MEA applications as a hermetic coating to prevent material degradation.
机译:植入式微电极阵列(MEAs)通过恢复假肢的通信和控制,为修复设备提供了临床前景。尽管多边环境协定的概念验证记录很有希望,但在动物模型中的工作表明,所获得的信号会随着时间的推移而退化。材料的坚固性和组织反应都被认为与设备寿命有关。非晶碳化硅(a-SiC)是一种耐腐蚀的坚固材料,它已成为可植入设备的替代封装层。我们通过组织组织反应中涉及的关键标志物的免疫组织化学表征,系统地检查了a-SiC涂层对Si探针的影响。植入后,我们在植入4周和8周后对神经元,星形胶质细胞和活化的小胶质细胞/巨噬细胞进行了设备捕获免疫组化标记。 Si和a-SiC涂层探针之间的神经元丢失和小胶质细胞活化相似,而植入a-SiC的组织显示出邻近探针的星形胶质细胞减少。这些结果表明,a-SiC具有与Si相似的生物相容性,并且可能适合作为可植入MEA应用的密封涂层以防止材料降解。

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