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新型紫杉醇载药胶束增强药物分子靶向递送,提高细胞毒性和逆转耐药性。

High cytotoxicity and resistant-cell reversal of novel paclitaxel loaded micelles by enhancing the molecular-target delivery of the drug.

机构信息

College of Pharmaceutical Sciences, Zhejiang University, Hangzhou 310058, People's Republic of China.

出版信息

Nanotechnology. 2007 Dec 12;18(49):495101. doi: 10.1088/0957-4484/18/49/495101. Epub 2007 Nov 2.

Abstract

Many antitumor drugs, such as paclitaxel (PTX), are widely used in cancer chemotherapy. However, their clinical use is limited by systemic toxicity, rapid blood clearance, and the occurrence of resistance. To increase the therapeutic index of these drugs, the antitumor drug PTX was encapsulated in novel micelles with glycolipid-like structure, which were formed by stearate grafted chitosan oligosaccharide in aqueous medium. The micelles could load the poorly soluble antitumor drug (PTX) with high entrapment efficiency and drug loading. PTX release was retarded as a result of the encapsulation of the micelles. PTX loaded micelles present excellent internalization into tumor cells as well as resistant cells and subsequently reside in cytoplasm, which results in increased intracellular accumulation of PTX in its molecular-target site. Consequently, cytotoxicity of PTX loaded micelles was improved sharply and resistant cells were reversed. In conclusion, high cytotoxicity can be obtained and resistant cells can be reversed by enhancing PTX's molecular-target delivery and accumulation via the encapsulation of the micelles. The present micelles are a promising carrier candidate for effective therapy of antitumor drugs with the target molecule in cytoplasm.

摘要

许多抗肿瘤药物,如紫杉醇(PTX),广泛应用于癌症化疗。然而,它们的临床应用受到全身毒性、快速血液清除和耐药性的限制。为了提高这些药物的治疗指数,将抗肿瘤药物 PTX 包封在具有类似糖脂结构的新型胶束中,该胶束由硬脂酸接枝壳寡糖在水介质中形成。胶束可以负载疏水性抗肿瘤药物(PTX),具有高包封效率和载药量。由于胶束的包封,PTX 的释放受到抑制。PTX 负载的胶束具有优异的内化进入肿瘤细胞以及耐药细胞的能力,并随后存在于细胞质中,导致 PTX 在其分子靶位的细胞内积累增加。因此,PTX 负载胶束的细胞毒性显著提高,耐药细胞被逆转。总之,通过增强 PTX 的分子靶向递释和通过胶束的包封来增加其在细胞质中的分子靶位的积累,可以获得高细胞毒性并逆转耐药细胞。目前的胶束是一种很有前途的载药候选物,可用于有效治疗细胞质中靶分子的抗肿瘤药物。

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