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Chimeric apoptotic bodies functionalized with natural membrane and modular delivery system for inflammation modulation

机译:用天然膜和模块化输送系统官能化的嵌合凋亡体,用于炎症调制

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Engineered extracellular vesicles (EVs) carrying therapeutic molecules are promising candidates for disease therapies. Yet, engineering EVs with optimal functions is a challenge that requires careful selection of functionally specific vesicles and a proper engineering strategy. Here, we constructed chimeric apoptotic bodies (cABs) for on-demand inflammation modulation by combining pure membrane from apoptotic bodies (ABs) as a bioconjugation/regulation module and mesoporous silica nanoparticles (MSNs) as a carrier module. MSNs were preloaded with anti-inflammatory agents (microRNA-21 or curcumin) and modified with stimuli-responsive molecules to achieve accurate cargo release at designated locations. The resulting cABs actively target macrophages in the inflammatory region and effectively promote M2 polarization of these macrophages to modulate inflammation due to the synergistic regulatory effects of AB membranes and the intracellular release of preloaded cargos. This work provides strategies to arbitrarily engineer modular EVs that integrate the advantages of natural EVs and synthetic materials for various applications.
机译:携带治疗分子的工程化细胞外囊(EVS)是疾病治疗的有希望的候选者。然而,具有最佳功能的工程EV是一个挑战,需要仔细选择功能特定的囊泡和适当的工程策略。在这里,我们通过将纯膜与凋亡/调节模块和介孔二氧化硅纳米颗粒(MSN)组合将纯膜与凋亡/调节模块(ABS)与凋亡/调节模块和作为载体模块的介孔二氧化硅纳米颗粒(MSN)组合,以满足点播炎症调节。 MSN与抗炎剂(MicroRNA-21或姜黄素)预加载,并用刺激响应分子修饰,以在指定位置达到准确的货物释放。所得到的驾驶室积极地靶向炎症区中的巨噬细胞,并有效地促进这些巨噬细胞的M2偏振,以调节炎症,因为AB膜的协同调节效果和预载的尸体的细胞内释放。这项工作为任意工程师的模块化EVS提供了策略,即集成了各种应用的天然EV和合成材料的优势。

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