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首页> 外文期刊>ACS nano >Multifunctional stable and pH-responsive polymer vesicles formed by heterofunctional triblock copolymer for targeted anticancer drug delivery and ultrasensitive MR imaging
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Multifunctional stable and pH-responsive polymer vesicles formed by heterofunctional triblock copolymer for targeted anticancer drug delivery and ultrasensitive MR imaging

机译:由杂功能三嵌段共聚物形成的多功能稳定且对pH有响应的聚合物囊泡,用于靶向抗癌药物递送和超灵敏MR成像

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摘要

A multifunctional stable and pH-responsive polymer vesicle nanocarrier system was developed for combined tumor-targeted delivery of an anticancer drug and superparamagnetic iron oxide (SPIO) nanoparticles (NPs). These multifunctional polymer vesicles were formed by heterofunctional amphiphilic triblock copolymers, that is, R (folate (FA) or methoxy)-poly(ethylene glycol)(M_w:5000)-poly(glutamate hydrozone doxorubicin)-poly(ethylene glycol) (M_w:2000)-acrylate (i.e., R (FA or methoxy)-PEG _(114)-P(Glu-Hyd-DOX)-PEG_(46)-acrylate). The amphiphilic triblock copolymers can self-assemble into stable vesicles in aqueous solution. It was found that the long PEG segments were mostly segregated into the outer hydrophilic PEG layers of the vesicles, thereby providing active tumor targeting via FA, while the short PEG segments were mostly segregated into the inner hydrophilic PEG layer of the vesicles, thereby making it possible to cross-link the inner PEG layer via the acrylate groups for enhanced in vivo stability. The therapeutic drug, DOX, was conjugated onto the polyglutamate segment, which formed the hydrophobic membrane of the vesicles using a pH-sensitive hydrazone bond to achieve pH-responsive drug release, while the hydrophilic SPIO NPs were encapsulated into the aqueous core of the stable vesicles, allowing for ultrasensitive magnetic resonance imaging (MRI) detection. The SPIO/DOX-loaded vesicles demonstrated a much higher r_2 relaxivity value than Feridex, a commercially available SPIO-based T_2 contrast agent, which was attributed to the high SPIO NPs loading level and the SPIO clustering effect in the aqueous core of the vesicles. Results from flow cytometry and confocal laser scanning microscopy (CLSM) analysis showed that FA-conjugated vesicles exhibited higher cellular uptake than FA-free vesicles which also led to higher cytotoxicity. Thus, these tumor-targeting multifunctional SPIO/DOX-loaded vesicles will provide excellent in vivo stability, pH-controlled drug release, as well as enhanced MRI contrast, thereby making targeted cancer therapy and diagnosis possible.
机译:开发了多功能稳定且对pH敏感的聚合物囊泡纳米载体系统,用于组合靶向肿瘤的抗癌药和超顺磁性氧化铁(SPIO)纳米粒子(NPs)的递送。这些多功能聚合物囊泡是由异官能两亲三嵌段共聚物形成的,即R(叶酸(FA)或甲氧基)-聚乙二醇(M_w:5000)-聚(谷氨酸氢盐阿霉素)-聚乙二醇(M_w :2000)-丙烯酸酯(即,R(FA或甲氧基)-PEG _(114)-P(Glu-Hyd-DOX)-PEG_(46)-丙烯酸酯)。两亲性三嵌段共聚物可以在水溶液中自组装成稳定的囊泡。发现长的PEG片段主要被分离到囊泡的亲水性PEG外层中,从而通过FA提供活性的肿瘤靶向,而短的PEG片段主要被分离到囊泡的亲水性PEG内层中,从而使其可能通过丙烯酸酯基交联内部PEG层,以增强体内稳定性。将治疗药物DOX偶联到聚谷氨酸片段上,该片段使用pH敏感的bond键形成囊泡的疏水膜以实现pH敏感药物的释放,而亲水性SPIO NP则被封装在马the的水核中囊泡,可进行超灵敏磁共振成像(MRI)检测。装载SPIO / DOX的囊泡比市售的基于SPIO的T_2造影剂Feridex表现出更高的r_2弛豫值,这归因于SPIO NPs的高装载水平和SPIO在囊泡水核中的聚集作用。流式细胞仪和共聚焦激光扫描显微镜(CLSM)分析的结果表明,与不含FA的囊泡相比,与FA偶联的囊泡显示出更高的细胞摄取,这也导致了更高的细胞毒性。因此,这些靶向肿瘤的多功能SPIO / DOX囊泡将提供出色的体内稳定性,pH控制的药物释放以及增强的MRI对比,从而使靶向癌症治疗和诊断成为可能。

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