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One-pot synthesis of hollow PDA@DOX nanoparticles for ultrasound imaging and chemo-thermal therapy in breast cancer

机译:空心PDA@DOX纳米颗粒的合成超声波成像和chemo-thermal疗法在乳腺癌

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摘要

Constructing nanocarriers with high drug loading capacity is a challenge, which limits the effective delivery of drugs to solid tumors. Here, we reported a one-pot synthesis of hollow nanoparticles (NPs) encapsulated by doxorubicin (DOX) and modified with polydopamine (PDA) to form PDA@DOX NPs for breast cancer treatment. PDA@DOX NPs demonstrated exceptionally high capacity (53.16%) for loading DOX. In addition, when PDA@DOX NPs were administered systemically, they exhibited responsive aggregation in the tumor sites and demonstrated a good controlled release effect for DOX due to the weak acidic environment of the tumor sites and targeting near-infrared (NIR) light irradiation. The PDA outer layer absorbed the near-infrared (NIR) light and facilitated simultaneous generation of heat energy for destroying the tumor cells to release the drug upon NIR irradiation. Moreover, this NIR-activated combined/ synergistic therapy exhibited remarkably complete tumor growth suppression in a breast cancer mouse model. Importantly, NPs exhibited a good ultrasound performance both in vitro and in vivo, which could monitor the treatment process. In conclusion, this NIR-activated PDA@DOX NP system is demonstrated as a good US-guided combination (chemotherapy + PTT) therapy platform with high loading capacity and controlled drug release characteristics, which is promising for the treatment of breast cancer.
机译:构建人们高药物加载能力是一个挑战,这限制了实体肿瘤的有效交付的药物。在这里,我们报告一锅法合成空心阿霉素纳米粒(NPs)封装(阿霉素)和修改polydopamine (PDA)形式PDA@DOX NPs乳腺癌的治疗。PDA@DOX NPs异常高容量负载阿霉素(53.16%)。PDA@DOX NPs管理系统时,他们表现出反应聚合肿瘤站点和展示了很好的控制释放效应对阿霉素由于弱酸性网站和目标环境的肿瘤近红外(NIR)光照射。外层吸收近红外(NIR)光和促进同步生成热能为破坏肿瘤细胞释放药物在近红外光谱辐照。这NIR-activated /协同治疗相结合表现出非常完整的肿瘤生长抑制乳腺癌小鼠模型。重要的是,NPs表现出良好的超声波性能在体外和体内可以监控治疗过程。结论,这NIR-activated PDA@DOX NP系统证明是一个好的US-guided组合吗(化疗+ PTT)治疗平台高装载容量和药物控制释放特点,是有前途的治疗乳腺癌。

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