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首页> 外文期刊>ACS applied materials & interfaces >Reactive Oxygen Species-Manipulated Drug Release from a Smart Envelope-Type Mesoporous Titanium Nanovehicle for Tumor Sonodynamic-Chemotherapy
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Reactive Oxygen Species-Manipulated Drug Release from a Smart Envelope-Type Mesoporous Titanium Nanovehicle for Tumor Sonodynamic-Chemotherapy

机译:活性氧从智能信封型介孔钛纳米载体中释放的药物用于肿瘤声动力学化学疗法。

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摘要

Despite advances in drug delivery systems (DDSs), the stimuli-responsive controlled release DDSs with high spatial/temporal resolution are still the best choice. Herein, a novel type of envelope-type mesoporous titanium dioxide nanoparticle (MTN) was developed for one-demand drug delivery platform. Docetaxel (DTX) was loaded in the pores of MTN with a high drug loading efficiency (similar to 2,6%). Then beta-cyclodextrin (beta-CD, a bulky gatekeeper) was attached to the outer surface of MTN via a reactive oxygen species (ROS) sensitive linker to block the pores (MTN@DTX-CD). MTN@DTX-CD could entrap the DTX in the pores and allow the rapid release until a focused ultrasound (US) emerged. A large number of ROS were generated by MTN under US radiation, leading to the cleavage of the ROS-sensitive linker; thus, DTX could be released rapidly since the gatekeepers (beta-CD) were detached. Besides, the generation of ROS could also be used for tumor-specific sonodynamic therapy (SDT). Studies have shown the feasibility of MTN@DTX-CD for US-triggered DTX release and sonodynamic-chemotherapy. In the in vitro and in vivo studies, by integrating SDT and chemotherapy into one system, MTN@DTX-CD showed excellent antitumor efficacy. More importantly, this novel DDS significantly decreased the side effects of DTX by avoiding the spleen and hematologic toxicity to tumor-bearing mice.
机译:尽管药物递送系统(DDS)有所进步,但具有高时空分辨率的刺激响应型控释DDS仍然是最佳选择。在这里,一种新型的包膜型介孔二氧化钛纳米粒子(MTN)被开发用于一种需求的药物递送平台。多西他赛(DTX)以较高的药物装载效率(接近2.6%)装载在MTN的孔中。然后,β-环糊精(β-CD,笨重的守门员)通过活性氧(ROS)敏感的连接剂连接到MTN的外表面,以阻塞孔(MTN @ DTX-CD)。 MTN @ DTX-CD可以将DTX截留在毛孔中并允许快速释放,直到出现聚焦超声(US)。 MTN在美国辐射下产生了大量的ROS,导致ROS敏感的连接子被裂解。因此,由于网守(beta-CD)被分离,DTX可以迅速释放。此外,ROS的产生也可用于肿瘤特异性声动力学治疗(SDT)。研究表明,MTN @ DTX-CD可用于美国触发的DTX释放和声动力化学疗法。在体外和体内研究中,通过将SDT和化学疗法整合到一个系统中,MTN @ DTX-CD显示出优异的抗肿瘤功效。更重要的是,这种新型DDS通过避免脾脏和血液对荷瘤小鼠的血液毒性,显着降低了DTX的副作用。

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