经颅直流电刺激改变了小鼠脑脊液-脑间质的交换。

IF 7.6 1区医学 Q1 CLINICAL NEUROLOGY

Brain Stimulation Pub Date : 2024-05-01 DOI:10.1016/j.brs.2024.04.009

Yan Wang, Hiromu Monai

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引用次数: 0

摘要

背景：经颅直流电刺激（tDCS）是一种非侵入性脑部刺激技术，近年来备受瞩目。临床研究已将经颅直流电刺激作为神经系统疾病康复的辅助手段，有证据表明它具有调节大脑清除机制的潜力。glymphatic系统是一种拟议的大脑废物清除系统，它认为脑脊液-间质（CSF-ISF）交换有助于有效清除代谢废物。虽然一些研究已将 tDCS 与星形胶质细胞的三磷酸肌醇（IP3）/Ca2+ 信号传导联系起来，但 tDCS 对 CSF-ISF 交换动态的影响仍不清楚。假设：tDCS 通过星形胶质细胞的 IP3/Ca2+ 信号传导影响 CSF-ISF 交换的动态：在本研究中，我们给用氯胺酮-氯丙嗪（KX）麻醉的 C57BL/6 小鼠注射了 tDCS（0.1mA，10 分钟）。阳极位于大脑皮层上方的颅骨上，阴极插入颈部。在 tDCS 之后，我们将生物素化葡聚糖胺（BDA）作为 CSF 示踪剂注入尾状腔（CM），直接评估脑液动态。然后在 30 或 60 分钟后提取大脑并固定。24 小时后，用 Alexa 594 结合的链霉亲和素（SA）对切片进行染色，用免疫组化方法观察 BDA。我们进行了脑电图（EEG）记录和水蒸发素 4（AQP4）/CD31 免疫染色，以研究 tDCS 的潜在机制。此外，我们还利用颈淋巴结成像技术监测了注射到蝶窦的伊文思蓝的外流。随后用三磷酸肌醇受体 2 型（IP3R2）剔除小鼠重复了这些实验：tDCS后，我们观察到CSF示踪剂流入量增加，这表明tDCS调节了CSF-ISF交换。此外，tDCS似乎还增强了大脑代谢废物的流出。脑电图记录显示，tDCS 后德尔塔波增加。结论：我们的研究结果表明，tDCS 可增强大脑代谢废物的排出：我们的研究结果表明，tDCS 可增强甘液系统的流入和流出。通过星形胶质细胞 IP3/Ca2+ 信号传导，tDCS 可改变δ波，而δ波与脑清除率呈正相关。这项研究强调了 tDCS 在调节大脑代谢废物清除方面的潜力。

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Transcranial direct current stimulation alters cerebrospinal fluid-interstitial fluid exchange in mouse brain

Background

Transcranial direct current stimulation (tDCS) is a non-invasive brain stimulation technique that has gained prominence recently. Clinical studies have explored tDCS as an adjunct to neurologic disease rehabilitation, with evidence suggesting its potential in modulating brain clearance mechanisms. The glymphatic system, a proposed brain waste clearance system, posits that cerebrospinal fluid-interstitial fluid (CSF-ISF) exchange aids in efficient metabolic waste removal. While some studies have linked tDCS to astrocytic inositol trisphosphate (IP₃)/Ca²⁺ signaling, the impact of tDCS on CSF-ISF exchange dynamics remains unclear.

Hypothesis

tDCS influences the dynamics of CSF-ISF exchange through astrocytic IP₃/Ca²⁺ signaling.

Methods

In this study, we administered tDCS (0.1 mA for 10 min) to C57BL/6N mice anesthetized with ketamine-xylazine (KX). The anode was positioned on the cranial bone above the cortex, and the cathode was inserted into the neck. Following tDCS, we directly assessed brain fluid dynamics by injecting biotinylated dextran amine (BDA) as a CSF tracer into the cisterna magna (CM). The brain was then extracted after either 30 or 60 min and fixed. After 24 h, the sectioned brain slices were stained with Alexa 594-conjugated streptavidin (SA) to visualize BDA using immunohistochemistry. We conducted Electroencephalography (EEG) recordings and aquaporin 4 (AQP4)/CD31 immunostaining to investigate the underlying mechanisms of tDCS. Additionally, we monitored the efflux of Evans blue, injected into the cisterna magna, using cervical lymph node imaging. Some experiments were subsequently repeated with inositol trisphosphate receptor type 2 (IP₃R2) knockout (KO) mice.

Results

Post-tDCS, we observed an increased CSF tracer influx, indicating a modulation of CSF-ISF exchange by tDCS. Additionally, tDCS appeared to enhance the brain's metabolic waste efflux. EEG recordings showed an increase in delta wave post-tDCS. But no significant change in AQP4 expression was detected 30 min post-tDCS. Besides, we found no alteration in CSF-ISF exchange and delta wave activity in IP₃R2 KO mice after tDCS.

Conclusion

Our findings suggest that tDCS augments the glymphatic system's influx and efflux. Through astrocytic IP₃/Ca²⁺ signaling, tDCS was found to modify the delta wave, which correlates positively with brain clearance. This study underscores the potential of tDCS in modulating brain metabolic waste clearance.

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来源期刊

Brain Stimulation 医学-临床神经学

CiteScore

13.10

自引率

9.10%

发文量

256

审稿时长

72 days

期刊介绍： Brain Stimulation publishes on the entire field of brain stimulation, including noninvasive and invasive techniques and technologies that alter brain function through the use of electrical, magnetic, radiowave, or focally targeted pharmacologic stimulation. Brain Stimulation aims to be the premier journal for publication of original research in the field of neuromodulation. The journal includes: a) Original articles; b) Short Communications; c) Invited and original reviews; d) Technology and methodological perspectives (reviews of new devices, description of new methods, etc.); and e) Letters to the Editor. Special issues of the journal will be considered based on scientific merit.