首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >A carrier-free dual-drug nanodelivery system functionalized with aptamer specific targeting HER2-overexpressing cancer cells
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A carrier-free dual-drug nanodelivery system functionalized with aptamer specific targeting HER2-overexpressing cancer cells

机译:一种无携带的双药纳米纳倍配送系统,其具有特异性靶向HER2-过度抑制癌细胞的适体特异性

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Exploration of a green carrier to avoid potential systemic toxicity and the unclear metabolic mechanism of traditional nanocarriers is of high importance for cancer therapy. Hence, we developed a carrier-free nanosystem for co-delivery of dual anti-cancer drugs ursolic acid (UA) and doxorubicin (DOX) using a "green'' and simple method. The co-assembled nanodrug was further modified with a HER2 aptamer by electrostatic interactions. The co-assembled dual nanodrug presented a spherical morphology with a uniform size (similar to 108.9 nm) and in a pH-triggered drug release manner. It made UA sensitize DOX to display synergistic anticancer effects at a low dose of DOX. Further, the aptamer surface decoration improved the intracellular drug retention of UA and DOX to as much as 2-fold in HER2 overexpressing cancer cells. In addition, the in vivo results further proved that the co-assembled nanodrug could significantly inhibit the tumor growth with a little side effects. In a word, this novel carrier-free dual-drug nanodelivery system could be a potential drug candidate for HER2 overexpressing cancer therapy, and UA could be used as a "green'' nanocarrier for delivery of hydrophobic drugs and fluorescent dyes in cancer treatment and diagnosis.
机译:探索绿色载体以避免潜在的全身毒性和传统纳米载波的不明确的代谢机制对于癌症治疗具有很高的重要性。因此,我们使用“绿色”和简单的方法开发了一种无携带的纳米纳米系统,用于共同递送双抗癌药物熊酸(UA)和多柔比星(DOX)。使用HER2进一步修饰共组合的纳米树脂通过静电相互作用的适体。共组合的双纳米树脂​​呈现具有均匀尺寸(类似于108.9nm)的球形形态,并以pH触发的药物释放方式呈现。它使DOX敏感,以低剂量显示协同抗癌效果进一步,Aptamer表面装饰将UA和Dox的细胞内药物保留改善在HER2过表达癌细胞中的2倍。此外,在体内结果进一步证明了共组合的纳米树质可以显着抑制肿瘤副作用略有生长。总之,这种新型无载体的双药纳米碳交付系统可以是HER2过表达癌症治疗的潜在药物候选者,UA可以用作DE的“绿色”纳米载波疏水性药物的制服和癌症治疗和诊断中的荧光染料。

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