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具有集成微流体的模型神经假体:一种控制反应性细胞和组织反应的潜在干预策略。

Model neural prostheses with integrated microfluidics: a potential intervention strategy for controlling reactive cell and tissue responses.

作者信息

Retterer Scott T, Smith Karen L, Bjornsson Christopher S, Neeves Keith B, Spence Andrew J H, Turner James N, Shain William, Isaacson Michael S

机构信息

Biomedical Engineering Program at Cornell University, Ithaca, NY 14853, USA.

出版信息

IEEE Trans Biomed Eng. 2004 Nov;51(11):2063-73. doi: 10.1109/TBME.2004.834288.

Abstract

Model silicon intracortical probes with microfluidic channels were fabricated and tested to examine the feasibility of using diffusion-mediated delivery to deliver therapeutic agents into the volume of tissue exhibiting reactive responses to implanted devices. Three-dimensional probe structures with microfluidic channels were fabricated using surface micromachining and deep reactive ion etching (DRIE) techniques. In vitro functional tests of devices were performed using fluorescence microscopy to record the transient release of Texas Red labeled transferrin (TR-transferrin) and dextran (TR-dextran) from the microchannels into 1% w/v agarose gel. In vivo performance was characterized by inserting devices loaded with TR-transferrin into the premotor cortex of adult male rats. Brain sections were imaged using confocal microscopy. Diffusion of TR-transferrin into the extracellular space and uptake by cells up to 400 microm from the implantation site was observed in brain slices taken 1 h postinsertion. The reactive tissue volume, as indicated by the presence of phosphorylated mitogen-activated protein kinases (MAPKs), was characterized using immunohistochemistry and confocal microscopy. The reactive tissue volume extended 600, 800, and 400 microm radially from the implantation site at 1 h, 24 h, and 6 weeks following insertion, respectively. These results indicate that diffusion-mediated delivery can be part of an effective intervention strategy for the treatment of reactive tissue responses around chronically implanted intracortical probes.

摘要

制造并测试了带有微流体通道的硅质皮质内探针模型,以检验使用扩散介导递送将治疗剂递送至对植入装置表现出反应性的组织区域的可行性。采用表面微加工和深反应离子刻蚀(DRIE)技术制造了具有微流体通道的三维探针结构。使用荧光显微镜对装置进行体外功能测试,以记录德克萨斯红标记的转铁蛋白(TR-转铁蛋白)和葡聚糖(TR-葡聚糖)从微通道向1% w/v琼脂糖凝胶中的瞬时释放。通过将装载有TR-转铁蛋白的装置插入成年雄性大鼠的运动前皮质来表征体内性能。使用共聚焦显微镜对脑切片进行成像。在插入后1小时获取的脑切片中,观察到TR-转铁蛋白扩散到细胞外空间并被距离植入部位达400微米的细胞摄取。使用免疫组织化学和共聚焦显微镜对由磷酸化丝裂原活化蛋白激酶(MAPK)的存在所指示的反应性组织区域进行表征。在插入后1小时、24小时和6周时,反应性组织区域分别从植入部位径向延伸600、800和400微米。这些结果表明,扩散介导递送可以成为治疗长期植入的皮质内探针周围反应性组织反应的有效干预策略的一部分。

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