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首页> 外文期刊>Theranostics >Bubble-Manipulated Local Drug Release from a Smart Thermosensitive Cerasome for Dual-Mode Imaging Guided Tumor Chemo-Photothermal Therapy
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Bubble-Manipulated Local Drug Release from a Smart Thermosensitive Cerasome for Dual-Mode Imaging Guided Tumor Chemo-Photothermal Therapy

机译:从智能热敏性药物中泡沫操纵的局部药物释放用于双模成像引导肿瘤化疗 - 光热疗法

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摘要

Thermosensitive liposomes have demonstrated great potential for tumor-specific chemotherapy. Near infrared (NIR) dyes loaded liposomes have also shown improved photothermal effect in cancer theranostics. However, the instability of liposomes often causes premature release of drugs or dyes, impeding their antitumor efficacy. Herein, we fabricated a highly stable thermo-responsive bubble-generating liposomal nanohybrid cerasome with a silicate framework, combined with a NIR dye to achieve NIR light stimulated, tumor-specific, chemo-photothermal synergistic therapy. Methods: In this system, NIR dye of 1,1'-Dioctadecyl-3,3,3',3'- Tetramethylindotricarbocyanine iodide (DiR) with long carbon chains was self-assembled with a cerasome-forming lipid (CFL) to encapsulate ammonium bicarbonate (ABC), which was further used for actively loading doxorubicin (DOX), affording a thermosensitive and photosensitive DOX-DiR@cerasome (ABC). Results: The resulting cerasome could disperse well in different media. Upon NIR light mediated thermal effect, ABC was decomposed to generate COsub2/sub bubbles, resulting in a permeable channel in the cerasome bilayer that significantly enhanced DOX release. After intravenous injection into tumor-bearing mice, DOX-DiR@cerasome (ABC) could be efficiently accumulated at the tumor tissue, as monitored by DiR fluorescence, lasting for more than 5 days. NIR light irradiation was then performed at 36h to locally heat the tumors, resulting in immediate COsub2/sub bubble generation, which could be clearly detected by ultrasound imaging, facilitating the monitoring process of controlled release of the drug. Significant antitumor efficacy could be obtained for the DOX-DiR@cerasome (ABC) + laser group, which was further confirmed by tumor tissue histological analysis.
机译:热敏脂质体已经表现出肿瘤特异性化学疗法的巨大潜力。近红外(NIR)染料载有脂质体也显示出癌症治疗癌中的显影效果。然而,脂质体的不稳定性通常会导致药物或染料过早释放,妨碍其抗肿瘤功效。在此,我们用硅酸盐框架制造了高度稳定的热响应气泡产生脂质体纳米嗜脂质体纳米含有型脂质体纳米含有型脂质体纳米含有型脂质体纳米混合物,与NIR染料结合以实现NIR光刺激,肿瘤特异性,化学光热协同疗法。方法:在该系统中,具有长碳链的1,1'-二恶英酰-3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3',3'-四甲基茚磺酰胺碘化锰(Dir),用半碳链进行自组装,用Culase的脂质(CFL)进行包封碳酸氢铵(ABC),其进一步用于主动装载多柔比星(DOX),得到热敏和光敏DOX-DIR @ cerasome(ABC)。结果:所得的CERASOME可以在不同介质中分散很好。在NIR光介导的热效应上,ABC被分解以产生CO 2 气泡,导致CERASOME双层中的可渗透通道,显着增强DOX释放。在静脉注射到肿瘤携带的小鼠之后,DOX-DIR @ CERASOME(ABC)可以在肿瘤组织中有效地积累,如通过荧光监测,持续超过5天。然后在36小时内进行NIR光照射,以局部加热肿瘤,导致立即CO 2 气泡产生,这可以通过超声成像清楚地检测,促进药物控制释放的监测过程。可以获得显着的抗肿瘤功效,用于DOX-DIR @ cirasome(ABC)+激光组,其通过肿瘤组织组织学分析进一步证实。

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