This study investigated relationships between a microscale neural probe's size and shape and its chronic reactive tissue response. Parylene-based probes were microfabricated with a thick shank (48 microm by 68 microm) and an integrated thin lateral platform (5 microm by 100 microm, either solid or one of three lattice sizes). Devices were implanted in rat cerebral cortex for 4 weeks before immunostaining for neurons, astrocytes, microglia, fibronectin, laminin, and neurofilament. While nonneuronal density (NND) generally increased and neuronal density decreased within 75 microm of a probe interface compared to unimplanted control regions, there were significant differential tissue responses within 25 microm of the platform's lateral edge compared to the shank. The NND in this region of the lateral edge was less than one-third of the corresponding region of the shank (129% and 425% increase, respectively). Moreover, neuronal density around the platform lateral edge was about one-third higher than at the shank (0.70 and 0.52 relative to control, respectively). Also, microglia reactivity and extracellular protein deposition was reduced at the lateral edge. There were no significant differences among platform designs. These results suggest that neural probe geometry is an important parameter for reducing chronic tissue encapsulation.

译文

:这项研究调查了微型神经探针的大小和形状与其慢性反应性组织反应之间的关系。使用厚柄(48微米乘68微米)和集成的薄侧平台(5微米乘100微米,实心或三个晶格大小之一)进行微加工,以聚对二甲苯为基础的探针。在对神经元,星形胶质细胞,小胶质细胞,纤连蛋白,层粘连蛋白和神经丝进行免疫染色之前,将装置植入大鼠大脑皮层4周。尽管与未植入的对照区域相比,非神经密度(NND)通常在探针界面的75微米之内增加而神经元密度降低,但与小腿相比,在平台侧边缘的25微米之内有明显的差异组织反应。在侧边缘的此区域中的NND小于柄的相应区域的三分之一(分别增加129%和425%)。此外,平台侧边缘周围的神经元密度比小腿高约三分之一(相对于对照分别为0.70和0.52)。同样,小胶质细胞反应性和细胞外蛋白质沉积在侧边缘减少。平台设计之间没有显着差异。这些结果表明,神经探针的几何形状是减少慢性组织包膜的重要参数。

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