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pH-Sensitive Nanoformulated Triptolide as a Targeted Therapeutic Strategy for Hepatocellular Carcinoma

机译:pH敏感的纳米级雷公藤甲素作为肝细胞癌的靶向治疗策略

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Hepatocellular carcinoma (HCC) has one of the worst prognoses for survival as it is poorly responsive to both conventional chemotherapy and mechanism-directed therapy. This results from a lack of therapeutic concentration in the tumor tissue coupled with the highly toxic off-site effects exhibited by these compounds. Consequently, we believe the best packaging for holistic therapy for HCC will involve three components: a potent therapeutic, a rationally designed drug delivery vehicle to enrich the target site concentration of the drug, and a surface ligand that can enable a greater propensity to internalization by tumor cells compared to the parenchyma. We screened a library containing hundreds of compounds against a panel of HCC cells and found the natural product, triptolide, to be more effective than sorafenib, doxorubicin, and daunorubicin, which are the current standards of therapy. However, the potential clinical application of triptolide is limited due to its poor solubility and high toxicity. Consequently, we synthesized tumor pH-sensitive nanoformulated triptolide coated with folate for use in an HCC-subpopulation that overexpresses the folate receptor. Our results show triptolide itself can prevent disease progression, but at the cost of significant toxicity. Conversely, our pH-sensitive nanoformulated triptolide facilitates uptake into the tumor, and specifically tumor cells, leading to a further increase in efficacy while mitigating systemic toxicity.
机译:肝细胞癌(HCC)的生存预后最差,因为它对常规化疗和机制指导治疗均反应不良。这是由于肿瘤组织中缺乏治疗浓度以及这些化合物所表现出的高毒性异位作用所致。因此,我们认为用于HCC整体治疗的最佳包装将包括三个部分:有效的治疗剂,合理设计的药物递送载体以丰富药物的目标部位浓度以及表面配体,该表面配体可通过以下方式更大程度地内化:肿瘤细胞与实质相比。我们筛选了一个包含数百种针对一组HCC细胞的化合物的文库,发现天然产物雷公藤内酯比索拉非尼,阿霉素和柔红霉素(目前的治疗标准)更有效。然而,雷公藤甲素的不良溶解性和高毒性使其潜在的临床应用受到限制。因此,我们合成了用叶酸包被的肿瘤pH敏感的纳米级雷公藤甲素,用于过表达叶酸受体的HCC亚群。我们的结果表明雷公藤甲素本身可以预防疾病进展,但以明显的毒性为代价。相反,我们对pH敏感的纳米级雷公藤内酯醇可促进肿瘤特别是肿瘤细胞的摄取,从而在降低全身毒性的同时进一步提高功效。

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