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Rationalizing the use of functionalized poly-lactic-co-glycolic acid nanoparticles for dendritic cell-based targeted anticancer therapy

机译:合理使用功能化的聚乳酸-乙醇酸纳米颗粒用于树突状细胞靶向抗癌治疗

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摘要

Background: Delivery of PLGA (poly [D, L-lactide-co-glycolide])-based biodegradable nanoparticles (NPs) to antigen presenting cells, particularly dendritic cells, has potential for cancer immunotherapy. Materials & methods: Using a PLGA NP vaccine construct CpG-NP-Tag (CpG-ODN-coated tumor antigen [Tag] encapsulating NP) prepared using solvent evaporation technique we tested the efficacy of ex vivo and in vivo use of this construct as a feasible platform for immune-based therapy. Results: CpG-NP-Tag NPs were avidly endocytosed and localized in the endosomal compartment of bone marrow-derived dendritic cells. Bone marrow-derived dendritic cells exposed to CpG-NP-Tag NPs exhibited an increased maturation (higher CD80/86 expression) and activation status (enhanced IL-12 secretion levels). In vivo results demonstrated attenuation of tumor growth and angiogenesis as well as induction of potent cytotoxic T-lymphocyte responses. Conclusion: Collectively, results validate dendritic cells stimulatory response to CpG-NP-Tag NPs (ex vivo) and CpG-NP-Tag NPs' tumor inhibitory potential (in vivo) for therapeutic applications, respectively.
机译:背景:基于PLGA(聚[D,L-丙交酯-乙交酯共聚物)的生物可降解纳米颗粒(NPs)的交付到抗原呈递细胞,特别是树突状细胞,具有癌症免疫治疗的潜力。材料和方法:使用通过溶剂蒸发技术制备的PLGA NP疫苗构建体CpG-NP-Tag(封装NP的CpG-ODN包被的肿瘤抗原[Tag]),我们测试了该构建体在体内和体外的药效。免疫治疗的可行平台。结果:CpG-NP-Tag NPs被内吞并定位在骨髓来源的树突状细胞的内体区室中。暴露于CpG-NP-Tag NPs的骨髓源性树突细胞表现出更高的成熟度(更高的CD80 / 86表达)和激活状态(增强的IL-12分泌水平)。体内结果证明了肿瘤生长和血管生成的减弱以及有效的细胞毒性T淋巴细胞反应的诱导。结论:总体而言,结果证实树突状细胞对CpG-NP-Tag NPs(离体)和CpG-NP-Tag NPs的肿瘤抑制潜力(体内)具有刺激性,可用于治疗应用。

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