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Alginic Acid-Coated Chitosan Nanoparticles Loaded with Legumain DNA Vaccine: Effect against Breast Cancer in Mice

机译:海藻酸涂层的壳聚糖纳米粒负载豆荚菌素DNA疫苗:对小鼠乳腺癌的影响。

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摘要

Legumain-based DNA vaccines have potential to protect against breast cancer. However, the lack of a safe and efficient oral delivery system restricts its clinical application. Here, we constructed alginic acid-coated chitosan nanoparticles (A.C.NPs) as an oral delivery carrier for a legumain DNA vaccine. First, we tested its characteristic in acidic environments in vitro. DNA agarose electrophoresis data show that A.C.NPs protected DNA better from degradation in acidic solution (pH 1.5) than did chitosan nanoparticles (C.NPs). Furthermore, size distribution analysis showed that A.C.NPs tended to aggregate and form micrometer scale complexes in pH<2.7, while dispersing into nanoparticles with an increase in pH. Mice were intragastrically administrated A.C.NPs carrying EGFP plasmids and EGFP expression was detected in the intestinal Peyer’s patches. Full-length legumain plasmids were loaded into different delivery carriers, including C.NPs, attenuated Salmonella typhimurium and A.C.NPs. A.C.NPs loaded with empty plasmids served as a control. Oral vaccination was performed in the murine orthotopic 4T1 breast cancer model. Our data indicate that tumor volume was significantly smaller in groups using A.C.NPs or attenuated Salmonella typhimurium as carriers. Furthermore, splenocytes co-cultured them with 4T1 cells pre-stimulated with CoCl2, which influenced the translocation of legumain from cytoplasm to plasma membrane, showed a 4.7 and 2.3 folds increase in active cytotoxic T lymphocytes (CD3+/CD8+/CD25+) when treated with A.C.NPs carriers compared with PBS C.NPs. Our study suggests that C.NPs coated with alginic acid may be a safe and efficient tool for oral delivery of a DNA vaccine. Moreover, a legumain DNA vaccine delivered orally with A.C.NPs can effectively improve autoimmune response and protect against breast cancer in mice.
机译:基于Legumain的DNA疫苗具有预防乳腺癌的潜力。但是,缺乏安全有效的口服给药系统限制了其临床应用。在这里,我们构建了藻酸包被的壳聚糖纳米颗粒(A.C.NPs)作为豆科植物DNA疫苗的口服载体。首先,我们在酸性环境中体外测试了其特性。 DNA琼脂糖电泳数据显示,与壳聚糖纳米颗粒(C.NPs)相比,A.C.NPs在酸性溶液(pH 1.5)中能更好地保护DNA免于降解。此外,粒度分布分析表明,在pH <2.7时,A.C.NPs易于聚集并形成微米级的络合物,而随着pH的增加而分散到纳米颗粒中。小鼠经胃内注射带有EGFP质粒的A.C.NP,并在肠道Peyer斑片中检测到EGFP的表达。全长豆科动物质粒被装载到不同的递送载体中,包括C.NP,减毒鼠伤寒沙门氏菌和A.C.NP。装有空质粒的A.C.NP用作对照。在鼠原位4T1乳腺癌模型中进行了口服疫苗接种。我们的数据表明,使用A.C.NPs或减毒鼠伤寒沙门氏菌作为载体的组中的肿瘤体积明显较小。此外,脾细胞与用CoCl2预刺激的4T1细胞共培养,这影响了豆荚菌素从细胞质到质膜的转运,显示活性细胞毒性T淋巴细胞分别增加了4.7和2.3倍(CD3 + / CD8 + / CD25 + )与PBS C.NPs相比,用ACNPs载体处理时。我们的研究表明,用海藻酸包被的C.NPs可能是口服DNA疫苗的安全有效工具。此外,口服A.C.NPs的豆科动物DNA疫苗可有效改善自身免疫反应并预防小鼠乳腺癌。

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