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Mitoxantrone-preloaded water-responsive phospholipid-amorphous calcium carbonate hybrid nanoparticles for targeted and effective cancer therapy

机译:尿催化剂预加载的水响应性磷脂 - 无定形碳酸钙杂种纳米粒子,用于靶向和有效癌症治疗

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Background: The application of mitoxantrone (MIT) in cancer therapy has been severely limited by its inherent drawbacks. In addition, effective cancer therapy calls for drug release systems capable of enforcing drug release within cancer cells in response to infinite stimulant with enhanced drug penetration capability. Methods: MIT-preloaded phospholipid-amorphous calcium carbonate hybrid nanoparticles (PL/ACC-MIT) that surface modified with PL shell (containing shielding polymer polyethylene glycol and targeting moiety folic acid) were prepared by a facile solvent-diffusion method. Results: It has been proven that the resulting PL/ACC-MIT nanoparticles demonstrated satisfactory stability against various aqueous environments with minimal drug leakage and exerted strong targeting capability but selective preference to the folate receptor-overexpressing cell line. In contrast, once exposed to the enzyme-abundant and acidic environments of cancer cells, the PL/ACC-MIT nanoparticles can readily decompose to facilitate quick drug release and enhanced drug penetration to yield preferable antitumor effect both in vitro and in vivo. Conclusion: In this study, MIT-preloaded water-responsive hybrid nanoparticles with increased stability, targetability, controlled drug release, and enhanced drug penetration were successfully developed, which might be a candidate for targeted and effective cancer therapy.
机译:背景:尿催化剂(MIT)在癌症治疗中的应用受到其固有缺点的严重限制。此外,有效的癌症治疗要求药物释放系统能够响应于无限兴奋剂而强化药物渗透能力的无限兴奋剂。方法:通过容易溶剂 - 扩散方法制备用Pl壳(含有屏蔽聚合物聚乙二醇和靶向部分叶酸)改性表面改性的MIT预加载的磷脂 - 无定形碳酸钙杂化纳米粒子(PL / ACC-MIT)。结果:已证明所得PL / ACC-MIT纳米粒子对各种水性环境的令人满意的稳定性令人满意,具有最小的药物泄漏,并且施加强烈的靶向能力,而是对叶酸受体过表达细胞的选择性偏好。相反,一旦暴露于癌细胞的酶 - 丰富和酸性环境,PL / ACC-MIT纳米颗粒可以容易地分解以促进快速药物释放和增强的药物渗透,以在体外和体内产生优选的抗肿瘤作用。结论:在本研究中,成功​​地开发了具有增加的稳定性,稳定性,受控药物释放和增强的药物渗透的麻省理工学院预载的水响应杂交纳米粒子,这可能是有针对性和有效的癌症治疗的候选者。

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