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The polyvinylpyrrolidone functionalized rGO/Bi2S3 nanocomposite as a near-infrared light-responsive nanovehicle for chemo-photothermal therapy of cancer

机译:功能化rGO聚乙烯吡咯烷酮/ Bi2S3纳米复合材料是近红外light-responsivenanovehicle chemo-photothermal治疗癌症

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摘要

Recently, a combination of chemotherapy with photothermal therapy (PTT) has received great attention for the construction of a near infrared (NIR)-controlled drug-delivery system for synergistic treatment of cancer, ultimately resulting in the enhancement of the therapeutic efficacy of anticancer drugs. Here, we developed a novel system for synergistic cancer therapy based on bismuth sulfide (Bi2S3) nanoparticle-decorated graphene functionalized with polyvinylpyrrolidone (PVP) (named PVP-rGO/Bi2S3). The as-prepared PVP-rGO/Bi2S3 nanocomposite has a high storage capacity for anticancer drugs (similar to 500% for doxorubicin (DOX)) and simultaneously has perfect photothermal conversion efficiency in the NIR region. The results of the in vitro accumulative drug release test manifests that the PVP-rGO/Bi2S3 nanocomposite could be applied as a dual pH-and NIR-responsive nanotherapeutic carrier for the controlled release of DOX from DOX-loaded PVP-rGO/Bi2S3 (PVP-rGO/Bi2S3@DOX). Moreover, the treatment of both cancer cells (including Hela, MCF-7, HepG2 and BEL-7402 cells) and BEL-7402 tumor-bearing mice with the PVP-rGO/Bi2S3@DOX complex followed by NIR laser irradiation produces significantly greater inhibition of cancer cell growth than the treatment with NIR irradiation alone or DOX alone, exhibiting a synergistic antitumor effect. Furthermore, due to the obvious NIR and X-ray absorption ability, the PVP-rGO/Bi2S3 nanocomposite could be employed as a dual-modal contrast agent for both photoacoustic tomography and X-ray computed tomography imaging. In addition to the good biocompatibility, the PVP-rGO/Bi2S3 nanocomposite paves a potential way for the fabrication of theranostic agents for dual-modal imaging-guided chemo-photothermal combined cancer therapy.
机译:最近,与化疗相结合的治疗方法光照疗法(PTT)已收到注意施工的近红外(NIR)控股药物传输系统协同治疗癌症,最终导致治疗的增强抗癌药物的效果。一个协同癌症治疗的新系统基于硫化铋(Bi2S3)nanoparticle-decorated石墨烯功能化与聚乙烯吡咯烷酮(PVP)(命名PVP-rGO / Bi2S3)。纳米复合材料具有高存储容量抗癌药物阿霉素(类似于500%(阿霉素)),同时也完美光热光谱分析在近红外光谱转换效率地区。药物释放测试体现PVP-rGO / Bi2S3纳米复合材料可以应用双重ph值和NIR-responsive nanotherapeutic的阿霉素控释载体此外,治疗癌症细胞(包括海拉、MCF-7 HepG2和bel - 7402细胞)和贝尔- 7402肿瘤小鼠的PVP-rGO / Bi2S3@DOX复杂的近红外激光紧随其后辐照产生显著更大抑制癌细胞的生长比使用近红外光谱辐照单独或阿霉素进行治疗孤独,表现出协同抗肿瘤效应。此外,由于明显的近红外光谱和x射线吸收能力,PVP-rGO / Bi2S3纳米复合材料可以采用dual-modal光声层析成像对比剂和x射线计算机断层扫描成像。除了良好的生物相容性,PVP-rGO / Bi2S3纳米复合材料为一个潜在的方法制造的theranostic代理dual-modal成像制导chemo-photothermal癌症治疗相结合。

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