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首页> 外文期刊>International Journal of Nanomedicine >Successful in vivo hyperthermal therapy toward breast cancer by Chinese medicine shikonin-loaded thermosensitive micelle
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Successful in vivo hyperthermal therapy toward breast cancer by Chinese medicine shikonin-loaded thermosensitive micelle

机译:中药加载热敏胶束对乳腺癌的体内高温治疗成功

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摘要

The Chinese traditional medicine Shikonin is an ideal drug due to its multiple targets to tumor cells. But in clinics, improving its aqueous solubility and tumor accumulation is still a challenge. Herein, a copolymer with tunable poly(N-isopropylacrymaide) and polylactic acid block lengths is designed, synthesized, and characterized in nuclear magnetic resonance. The corresponding thermosensitive nanomicelle (TN) with well-defined core-shell structure is then assembled in an aqueous solution. For promoting the therapeutic index, the physical-chemistry properties of TNs including narrow size, low critical micellar concentration, high serum stability, tunable volume phase transition temperature (VPTT), high drug-loading capacity, and temperature-controlled drug release are systematically investigated and regulated through the fine self-assembly. The shikonin is then entrapped in a degradable inner core resulting in a shikonin-loaded thermosensitive nanomicelle (STN) with a VPTT of ~40°C. Compared with small-molecular shikonin, the in vitro cellular internalization and cytotoxicity of STN against breast cancer cells (Michigan Cancer Foundation-7) are obviously enhanced. In addition, the therapeutic effect is further enhanced by the programmed cell death (PCD) specifically evoked by shikonin. Interestingly, both the proliferation inhibition and PCD are synergistically promoted as T > VPTT, namely the temperature-regulated passive targeting. Consequently, as intravenous injection is administered to the BALB/c nude mice bearing breast cancer, the intra-tumor accumulation of STNs is significantly increased as T > VPTT, which is regulated by the in-house developed heating device. The in vivo antitumor assays against breast cancer further confirm the synergistically enhanced therapeutic efficiency. The findings of this study indicate that STN is a potential effective nanoformulation in clinical cancer therapy.
机译:中国传统医学Shikonin是一种理想的药物,由于其对肿瘤细胞的多种靶标。但在诊所,改善其水溶性和肿瘤积累仍然是一个挑战。在此,设计,合成,合成,合成,具有可调谐聚(N-异丙基丙烯酸酯)和聚乳酸块长度的共聚物。然后在水溶液中组装具有明确定义的核壳结构的相应热敏纳米摩尔(TN)。为了促进治疗指数,系统地,系统地研究了包括窄尺寸,低临界胶束浓度,高血清稳定性,可调体积相变温度(VPTT),高药物负载能力和温度控制的药物释放的TNS的物理化学性质并通过细制的自我组装管制。然后将Shikonin捕获在可降解的内核中,导致ShikoNin加载的热敏纳米摩尔(STN),VPTT为〜40℃。与小分子什莲素相比,显然增强了对乳腺癌细胞(密歇根癌基础-7)的体外细胞内化和细胞毒性。此外,通过Shikonin专门引起的编程细胞死亡(PCD)进一步增强了治疗效果。有趣的是,增殖抑制和PCD都是协同促进为T> VPTT的,即温度调节的被动靶向。因此,随着静脉注射给患有乳腺癌的Balb / C裸鼠施用,STN的肿瘤内积累明显增加,如图所开发的加热装置的内部调节。对乳腺癌的体内抗肿瘤测定进一步证实了协同增强的治疗效率。该研究的结果表明,STN是临床癌症治疗中的潜在有效的纳米造型体。

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