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芯片上研究磁刺激对玻璃和纳米多孔表面上单个神经细胞活力和增殖的影响。

On-Chip Studies of Magnetic Stimulation Effect on Single Neural Cell Viability and Proliferation on Glass and Nanoporous Surfaces.

出版信息

ACS Appl Mater Interfaces. 2018 Aug 29;10(34):28269-28278. doi: 10.1021/acsami.8b05715. Epub 2018 Aug 20.

DOI:10.1021/acsami.8b05715
PMID:30080968
Abstract

Transcranial magnetic stimulation (TMS) is a noninvasive neuromodulation technique, an FDA-approved treatment method for various neurological disorders such as depressive disorder, Parkinson's disease, post-traumatic stress disorder, and migraine. However, information concerning the molecular/cellular-level mechanisms of neurons under magnetic simulation (MS), particularly at the single neural cell level, is still lacking, resulting in very little knowledge of the effects of MS on neural cells. In this paper, the effects of MS on the behaviors of neural cell N27 at the single-cell level on coverslip glass substrate and anodic aluminum oxide (AAO) nanoporous substrate are reported for the first time. First, it has been found that the MS has a negligible cytotoxic effect on N27 cells. Second, MS decreases nuclear localization of paxillin, a focal adhesion protein that is known to enter the nucleus and modulate transcription. Third, the effect of MS on N27 cells can be clearly observed over 24 h, the duration of one cell cycle, after MS is applied to the cells. The size of cells under MS was found to be statistically smaller than that of cells without MS after one cell cycle. Furthermore, directly monitoring cell division process in the microholders on a chip revealed that the cells under MS generated statistically more daughter cells in one average cell cycle time than those without MS. All these results indicate that MS can affect the behavior of N27 cells, promoting their proliferation and regeneration.

摘要

经颅磁刺激(TMS)是一种非侵入性神经调节技术,已被美国食品和药物管理局(FDA)批准用于治疗多种神经疾病,如抑郁症、帕金森病、创伤后应激障碍和偏头痛。然而,关于磁模拟(MS)下神经元的分子/细胞水平机制的信息仍然缺乏,这导致对 MS 对神经细胞的影响知之甚少。在本文中,首次报道了 MS 对覆盖玻片玻璃基底和阳极氧化铝(AAO)纳米多孔基底上的神经细胞 N27 单细胞水平行为的影响。首先,已经发现 MS 对 N27 细胞几乎没有细胞毒性作用。其次,MS 减少了黏着斑蛋白 paxillin 的核定位,黏着斑蛋白是一种已知进入细胞核并调节转录的焦点黏附蛋白。第三,在将 MS 施加到细胞后,可以在 24 小时内,即一个细胞周期的持续时间内,清楚地观察到 MS 对 N27 细胞的影响。发现在一个细胞周期后,MS 下的细胞大小明显小于没有 MS 的细胞。此外,在芯片上的微室中直接监测细胞分裂过程表明,在一个平均细胞周期时间内,MS 下的细胞产生的子细胞数量统计上多于没有 MS 的细胞。所有这些结果表明,MS 可以影响 N27 细胞的行为,促进其增殖和再生。

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