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原位质谱成像技术用于阐明腺苷 A 受体激动剂和阿普唑仑对睡眠调节的影响。

In Situ Mass Spectrometry Imaging to Elucidate the Effects of an Adenosine A Receptor Agonist and Alprazolam on Sleep Regulation.

作者信息

Zhang Yi, Yang Guixiang, Jin Qian, Shi Tong, Chen Xuejun, Zhang Ruihua, Wang Chen, Li Liqin

机构信息

State Key Laboratory of NBC Protection for Civilian, Beijing 102205, China.

出版信息

ACS Pharmacol Transl Sci. 2025 Feb 20;8(3):841-853. doi: 10.1021/acsptsci.4c00707. eCollection 2025 Mar 14.

Abstract

Alprazolam (Alp), a commonly used sleep medication in clinical practice, has several potential limitations, including a narrow therapeutic dosage range and a delayed sleep onset. CGS21680 (CGS), a selective agonist of the adenosine A receptor, exhibits neuroinhibitory properties. This study aimed to evaluate the effects of CGS on the sleep properties of Alp. The sleep-inducing effects of Alp were assessed through the righting reflex, while the sedative effects of CGS were evaluated by spontaneous activity detection. The synergistic effect of CGS on Alp was evaluated by using electroencephalography and electromyography. The results indicate that we optimized and selected ED dose of Alp and ED dose of CGS for coadministration. CGS reduced the sleep latency induced by Alp and extended the sleep duration. The distribution of Alp in the brain was assessed through mass spectrometry imaging (MSI). The blood-brain barrier (BBB) model was established to evaluate the impact of CGS on the transmittance of Alp. The results indicated that CGS influenced the distribution of Alp across various brain regions and increased Alp's transmittance across the BBB. The metabolic pathways of GABA, glutamate, and glutamine were assessed through MSI and enzyme activity verification. The coadministration of Alp and CGS resulted in the regulation of GABA, glutamate, and glutamine during the sleep latency and sleep maintenance periods, respectively. In conclusion, the potentiating effect of CGS on the sleep-inducing properties of Alp is attributed to its ability to modulate the distribution of Alp in the brain by enhancing BBB permeability and its influence on Alp-induced neurotransmitter release.

摘要

阿普唑仑(Alp)是临床实践中常用的睡眠药物,有几个潜在的局限性,包括治疗剂量范围窄和睡眠起效延迟。CGS21680(CGS)是腺苷A受体的选择性激动剂,具有神经抑制特性。本研究旨在评估CGS对Alp睡眠特性的影响。通过翻正反射评估Alp的促睡眠作用,通过自发活动检测评估CGS的镇静作用。利用脑电图和肌电图评估CGS对Alp的协同作用。结果表明,我们优化并选择了Alp的有效剂量和CGS的有效剂量进行联合给药。CGS缩短了Alp诱导的睡眠潜伏期并延长了睡眠时间。通过质谱成像(MSI)评估Alp在大脑中的分布。建立血脑屏障(BBB)模型以评估CGS对Alp透过率的影响。结果表明,CGS影响Alp在各个脑区的分布,并增加Alp穿过血脑屏障的透过率。通过MSI和酶活性验证评估γ-氨基丁酸(GABA)、谷氨酸和谷氨酰胺的代谢途径。Alp和CGS联合给药分别在睡眠潜伏期和睡眠维持期导致GABA、谷氨酸和谷氨酰胺的调节。总之,CGS对Alp促睡眠特性的增强作用归因于其通过增强血脑屏障通透性来调节Alp在大脑中的分布的能力及其对Alp诱导的神经递质释放的影响。

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