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MR imaging tracking of inflammation-activatable engineered neutrophils for targeted therapy of surgically treated glioma

机译:MR成像追踪可炎症激活的工程中性粒细胞用于靶向治疗手术治疗的神经胶质瘤

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摘要

Cell-based drug delivery systems have shown promising capability for tumor-targeted therapy owing to the intrinsic tumor-homing and drug-carrying property of some living cells. However, imaging tracking of their migration and bio-effects is urgently needed for clinical application, especially for glioma. Here, we report the inflammation-activatable engineered neutrophils by internalizing doxorubicin-loaded magnetic mesoporous silica nanoparticles (ND-MMSNs) which can provide the potential for magnetic resonance (MR) imaging tracking of the drug-loaded cells to actively target inflamed brain tumor after surgical resection of primary tumor. The phagocytized D-MMSNs possess high drug loading efficiency and do not affect the host neutrophils’ viability, thus remarkably improving intratumoral drug concentration and delaying relapse of surgically treated glioma. Our study offers a new strategy in targeted cancer theranostics through combining the merits of living cells and nanoparticle carriers.
机译:由于某些活细胞固有的肿瘤归巢和载药特性,基于细胞的药物递送系统已显示出有针对性的靶向肿瘤治疗能力。然而,对于临床应用,特别是对于神经胶质瘤,迫切需要对它们的迁移和生物效应进行成像跟踪。在这里,我们报告通过内化负载阿霉素的磁性介孔二氧化硅纳米颗粒(ND-MMSNs)来激活炎症激活的中性粒细胞,这可以为药物加载细胞的磁共振(MR)成像追踪提供潜力,从而在治疗后主动靶向发炎的脑肿瘤手术切除原发肿瘤。吞噬的D-MMSN具有较高的载药效率,并且不影响宿主中性粒细胞的生存能力,因此显着提高了瘤内药物浓度并延迟了手术治疗的神经胶质瘤的复发。我们的研究通过结合活细胞和纳米颗粒载体的优点,提供了靶向癌症治疗学的新策略。

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