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易于工程化的巨噬细胞衍生外泌体功能化 PLGA 纳米载体,通过调节卒中后抑郁大鼠模型中小胶质细胞极化,实现双重药物配方的靶向递送。

Facile engineered macrophages-derived exosomes-functionalized PLGA nanocarrier for targeted delivery of dual drug formulation against neuroinflammation by modulation of microglial polarization in a post-stroke depression rat model.

机构信息

Department of Neurology,Ningbo Medical Center Lihuili Hospital, Ningbo University, Ningbo, Zhejiang 315040, China.

School of Pharmaceutical Sciences, Wenzhou Medical University, Wenzhou, Zhejiang 325035, China.

出版信息

Biomed Pharmacother. 2024 Oct;179:117263. doi: 10.1016/j.biopha.2024.117263. Epub 2024 Sep 8.

DOI:10.1016/j.biopha.2024.117263
PMID:39243431
Abstract

Post-stroke depression (POSD) is a common difficulty and most predominant emotional syndrome after stroke often consequences in poor outcomes. In the present investigation, we have designed and studied the neurologically active celastrol/minocycline encapsulated with macrophages-derived exosomes functionalized PLGA nanoformulations (CMC-EXPL) to achieve enhanced anti-inflammatory behaviour and anti-depressant like activity in a Rat model of POSD. The animal model of POSD was established through stimulating process with chronic unpredictable mild stress (CUM) stimulations after procedure of middle cerebral artery occlusion (MCAO). Neuronal functions and Anti-inflammation behaviours were observed by histopathological (H&E) examination and Elisa analyses, respectively. The anti-depressive activity of the nanoformulations treated Rat models were evaluated by open-field and sucrose preference test methods. Microglial polarization was evaluated via flow-cytometry and qRT-PCR observations. The observed results exhibited that prepared nanoformulations reduced the POSD-stimulated depressive-like activities in rat models as well alleviated the neuronal damages and inflammatory responses in the cerebral hippocampus. Importantly, prepared CMC-EXPL nanoformulation effectively prevented the M1 pro-inflammatory polarization and indorsed M2 anti-inflammatory polarization, which indicates iNOS and CD86 levels significantly decreased and upsurged Arg-1 and CD206 levels. CMC-EXPL nanoformulation suggestively augmented anti-depressive activities and functional capability and also alleviated brain inflammation in POSD rats, demonstrating its therapeutic potential for POSD therapy.

摘要

中风后抑郁症(POSD)是中风后常见的困难和最主要的情绪综合征,通常导致不良结局。在本研究中,我们设计并研究了载有巨噬细胞衍生的外泌体功能化 PLGA 纳米制剂的 Celastrol/米诺环素(CMC-EXPL),以在 POSD 大鼠模型中实现增强的抗炎行为和抗抑郁样活性。通过在大脑中动脉闭塞(MCAO)后进行慢性不可预测的轻度应激(CUM)刺激过程,建立 POSD 动物模型。通过组织病理学(H&E)检查和 Elisa 分析分别观察神经元功能和抗炎行为。通过旷场和蔗糖偏好测试方法评估纳米制剂处理的大鼠模型的抗抑郁活性。通过流式细胞术和 qRT-PCR 观察评估小胶质细胞极化。观察结果表明,所制备的纳米制剂减轻了大鼠模型中 POSD 刺激的抑郁样活性,同时减轻了大脑海马区的神经元损伤和炎症反应。重要的是,所制备的 CMC-EXPL 纳米制剂有效地防止了 M1 促炎极化,并促进了 M2 抗炎极化,这表明 iNOS 和 CD86 水平显著降低,Arg-1 和 CD206 水平升高。CMC-EXPL 纳米制剂增强了抗抑郁活性和功能能力,并减轻了 POSD 大鼠的脑炎症,表明其在 POSD 治疗中的治疗潜力。

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引用本文的文献

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Engineering small extracellular vesicles: Unlocking the brain's secret passage for central nervous system therapies.工程化小细胞外囊泡:开启用于中枢神经系统治疗的大脑秘密通道。
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