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与成年大鼠相比,年轻大鼠的神经植入物的炎症异物反应显著降低,记录性能得到改善。

Significantly reduced inflammatory foreign-body-response to neuroimplants and improved recording performance in young compared to adult rats.

机构信息

Department of Neurobiology, the Alexander Silberman Institute of Life Science, the Hebrew University of Jerusalem, Jerusalem, Israel; The Charles E. Smith Family and Prof. Joel Elkes Laboratory for Collaborative Research in Psychobiology, the Hebrew University of Jerusalem, Jerusalem, Israel.

Department of Neurobiology, the Alexander Silberman Institute of Life Science, the Hebrew University of Jerusalem, Jerusalem, Israel; The Charles E. Smith Family and Prof. Joel Elkes Laboratory for Collaborative Research in Psychobiology, the Hebrew University of Jerusalem, Jerusalem, Israel; Edmond and Lily Safra Center for Brain Sciences, the Hebrew University of Jerusalem, Jerusalem, Israel.

出版信息

Acta Biomater. 2023 Mar 1;158:292-307. doi: 10.1016/j.actbio.2023.01.002. Epub 2023 Jan 9.

Abstract

The multicellular inflammatory encapsulation of implanted intracortical multielectrode arrays (MEA) is associated with severe deterioration of their field potentials' (FP) recording performance, which thus limits the use of brain implants in basic research and clinical applications. Therefore, extensive efforts have been made to identify the conditions in which the inflammatory foreign body response (FBR) is alleviated, or to develop methods to mitigate the formation of the inflammatory barrier. Here, for the first time, we show that (1) in young rats (74±8 gr, 4 weeks old at the onset of the experiments), cortical tissue recovery following MEA implantation proceeds with ameliorated inflammatory scar as compared to adult rats (242 ± 18 gr, 9 weeks old at the experimental onset); (2) in contrast to adult rats in which the Colony Stimulating factor 1 Receptor (CSF1R) antagonist chow eliminated ∼95% of the cortical microglia but not microglia adhering to the implant surfaces, in young rats the microglia adhering to the implant were eliminated along with the parenchymal microglia population. The removal of microglia adhering to the implant surfaces was correlated with improved recording performance by in-house fabricated Perforated Polyimide MEA Platforms (PPMP). These results support the hypothesis that microglia adhering to the surface of the electrodes, rather than the multicellular inflammatory scar, is the major underlying mechanism that deteriorates implant recording performance, and that young rats provide an advantageous model to study months-long, multisite electrophysiology in freely behaving rats. STATEMENT OF SIGNIFICANCE: Multisite electrophysiological recordings and stimulation devices play central roles in basic brain research and medical applications. The insertion of multielectrode-array platforms into the brain's parenchyma unavoidably injures the tissue, and initiates a multicellular inflammatory cascade culminating in the formation of an encapsulating scar tissue (the foreign body response-FBR). The dominant view, which directs most current research efforts to mitigate the FBR, holds that the FBR is the major hurdle to effective electrophysiological use of neuroprobes. By contrast, this report demonstrates that microglia adhering to the surface of a neuroimplants, rather than the multicellular FBR, underlie the performance deterioration of neuroimplants. These findings pave the way to the development of novel and focused strategies to overcome the functional deterioration of neuroimplants.

摘要

植入皮层内多电极阵列(MEA)的多细胞炎症包裹与场电位(FP)记录性能的严重恶化有关,这限制了脑植入物在基础研究和临床应用中的使用。因此,人们已经做出了广泛的努力来确定减轻炎症异物反应(FBR)的条件,或者开发减轻炎症屏障形成的方法。在这里,我们首次表明:(1)在年轻大鼠(74±8 克,实验开始时 4 周龄)中,与成年大鼠(242±18 克,实验开始时 9 周龄)相比,MEA 植入后皮质组织的恢复过程中炎症疤痕得到了改善;(2)与成年大鼠相反,在成年大鼠中,集落刺激因子 1 受体(CSF1R)拮抗剂饮食消除了约 95%的皮质小胶质细胞,但没有消除附着在植入物表面的小胶质细胞,在年轻大鼠中,附着在植入物上的小胶质细胞与实质小胶质细胞群体一起被消除。附着在植入物表面的小胶质细胞的去除与内部制造的穿孔聚酰亚胺 MEA 平台(PPMP)的记录性能的改善相关。这些结果支持这样的假设,即附着在电极表面上的小胶质细胞,而不是多细胞炎症疤痕,是导致植入物记录性能恶化的主要潜在机制,并且年轻大鼠为研究自由活动大鼠中长达数月的多部位电生理学提供了有利的模型。

意义声明

多部位电生理记录和刺激装置在基础脑研究和医学应用中起着核心作用。多电极阵列平台插入大脑实质不可避免地会损伤组织,并引发多细胞炎症级联反应,最终形成包裹性疤痕组织(异物反应-FBR)。目前大多数研究工作的主导观点是减轻 FBR,认为 FBR 是有效利用神经探针进行电生理的主要障碍。相比之下,本报告表明,附着在神经植入物表面的小胶质细胞,而不是多细胞 FBR,是神经植入物性能恶化的基础。这些发现为开发克服神经植入物功能恶化的新的、有针对性的策略铺平了道路。

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