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Doxorubicin-Conjugated PAMAM Dendrimers for pH-Responsive Drug Release and Folic Acid-Targeted Cancer Therapy

机译:阿霉素缀合的PAMAM树状大分子用于pH响应药物释放和叶酸靶向的癌症治疗

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We present here the development of multifunctional doxorubicin (DOX)-conjugated poly(amidoamine) (PAMAM) dendrimers as a unique platform for pH-responsive drug release and targeted chemotherapy of cancer cells. In this work, we covalently conjugated DOX onto the periphery of partially acetylated and folic acid (FA)-modified generation 5 (G5) PAMAM dendrimers through a pH-sensitive cis -aconityl linkage to form the G5.NHAc-FA-DOX conjugates. The formed dendrimer conjugates were well characterized using different methods. We show that DOX release from the G5.NHAc-FA-DOX conjugates follows an acid-triggered manner with a higher release rate under an acidic pH condition (pH = 5 or 6, close to the acidic pH of tumor microenvironment) than under a physiological pH condition. Both in vitro cytotoxicity evaluation and cell morphological observation demonstrate that the therapeutic activity of dendrimer-DOX conjugates against cancer cells is absolutely related to the DOX drug released. More importantly, the FA conjugation onto the dendrimers allowed a specific targeting to cancer cells overexpressing FA receptors (FAR), and allowed targeted inhibition of cancer cells. The developed G5.NHAc-FA-DOX conjugates may be used as a promising nanodevice for targeted cancer chemotherapy.
机译:我们在此介绍多功能阿霉素(DOX)结合的聚(酰胺基胺)(PAMAM)树状大分子的开发,作为pH响应药物释放和癌细胞靶向化疗的独特平台。在这项工作中,我们通过pH敏感的顺式-乙酰金属键将DOX共价缀合到部分乙酰化和叶酸(FA)修饰的第5代(G5)PAMAM树状聚合物的外围,形成G5.NHAc-FA-DOX缀合物。使用不同的方法可以很好地表征形成的树状聚合物共轭物。我们显示从G5.NHAc-FA-DOX缀合物释放的DOX遵循酸触发方式,在酸性pH条件(pH = 5或6,接近肿瘤微环境的酸性pH)下的释放速率高于在酸性条件下的释放速率。生理pH条件。体外细胞毒性评估和细胞形态学观察均表明,树状聚合物-DOX缀合物对癌细胞的治疗活性与释放的DOX药物绝对相关。更重要的是,与树状聚合物结合的FA可以特异性靶向过表达FA受体(FAR)的癌细胞,并可以靶向抑制癌细胞。开发的G5.NHAc-FA-DOX偶联物可用作靶向癌症化疗的有前途的纳米装置。

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