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Crosslinked self-assembled nanoparticles for chemo-sonodynamic combination therapy favoring antitumor, antimetastasis management and immune responses

机译:用于化疗的交联自组装纳米粒子,用于化疗抗肿瘤,抗肿瘤,抗炎和免疫应答

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Sonodynamic therapy (SDT) has been proposed as a new modality for cancer management through low-intensity ultrasound induced activation of sonosensitizers. Here, we designed a novel redox/enzyme/ultrasound responsive chondroitin sulfate-chlorin e6-lipoic acid nanoplatform loading docetaxel, combining SDT and chemotherapy, for antiproliferation and antimetastasis of melanoma. The reversibly crosslinked and self-assembled nanoparticles possessed monodispersive size distribution, stability in physical conditions, while showing increased uptake with rapid drug release in simulated tumor microenvironment (reductive potentials and degradative hyaluronidase-1). With synthesized ultrasound sensitive polymer backbones, SDT induced the generation of cellular reactive oxygen species and mitochondrial damage, exerting the apoptotic effect through the release of cytochrome C, the expression of cleaved caspase-9 followed by the functional cleaved caspase-3. Chemo-sonodynamic therapy not only inhibited tumor growth and metastasis with reduced metastatic protein expression, but also caused immune response via the release of tumor-associated antigens. It was initially demonstrated that SDT could induce the tumor cell death, therefore having potentials to recruit cytotoxic lymphocytes into tumor sites. Notably, the nanoplatforms exhibited good in vivo stability and blood compatibility, indicating the safety and efficiency in drug delivery. Our work thus presents a convenient approach to fabricate intelligent multifunctional nanoparticles and paves a path for effective cancer therapies.
机译:通过低强度超声诱导的超声溶解器激活,已经提出了Sonodynamic Therapication(SDT)作为癌症管理的一种新型癌症管理。在这里,我们设计了一种新型氧化还原/酶/超声响应性软骨素硫酸盐 - 氯e6-硫辛酸纳米酮素加载多西紫杉醇,组合SDT和化疗,用于黑色素瘤的抗溶解和抗体抗体。可逆交联和自组装的纳米颗粒具有单双相尺寸分布,物理条件的稳定性,同时显示模拟肿瘤微环境中的快速药物释放的增加(还原电位和降解透明质酸酶-1)。通过合成的超声敏感聚合物骨架,SDT诱导细胞反应性氧物质和线粒体损伤的产生,通过细胞色素C的释放来施加凋亡效果,切割的Caspase-9的表达,然后是功能性切割的Caspase-3。化学 - 声学疗法不仅抑制肿瘤生长和转移,转移蛋白表达降低,而且通过释放肿瘤相关抗原引起免疫应答。最初证明SDT可以诱导肿瘤细胞死亡,因此具有促进细胞毒性淋巴细胞进入肿瘤部位的潜力。值得注意的是,纳米纳薄形式在体内稳定性和血液兼容性方面表现出良好,表明药物递送的安全性和效率。因此,我们的工作提出了一种方便的方法来制造智能多功能纳米粒子,铺平了一种有效的癌症疗法的路径。

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