首页> 外文期刊>Saudi Pharmaceutical Journal >Effect simultaneous delivery with P-glycoprotein inhibitor and nanoparticle administration of doxorubicin on cellular uptake and in vitro anticancer activity
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Effect simultaneous delivery with P-glycoprotein inhibitor and nanoparticle administration of doxorubicin on cellular uptake and in vitro anticancer activity

机译:用P-糖蛋白抑制剂和纳米粒子施用多柔比蛋白同时递送多霉素对细胞吸收和体外抗癌活性的影响

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摘要

Multidrug resistance (MDR) is the most common problem of inadequate therapeutic response in tumor cells. Many trials has been developed to overcome drug efflux by P-glycoprotein (P-gp). For instance, co-administration of a number of drugs called chemosensitizers or MDR modulators with a chemotherapeutic agent to inhibit drug efflux. But for optimal synergy, the drug and inhibitor combination may need to be temporally colocalized in the tumor cells. In this study, we encapsulated the Ver and Dox in PLGA nanoparticles to inhibit the P-gp drug efflux in breast cancer. Moreover, the effect of either Dox solution (Dox S ), Dox nanoparticles (Dox NP ), Dox S ?+?Ver S , Dox NP ?+?Ver S , Dox NP ?+?Ver NP or Dox-Ver NP was evaluated. It was found that co administration of Dox NP with Ver NP (70.76%) showed similar cellular uptake of Dox to Dox/Ver combination solution (70.62%). However it is observed that Dox NP ?+?Ver NP has the highest apoptotic activity (early apoptotic 13.52?±?0.06%, late apoptotic 53.94?±?0.15%) on human breast adenocarcinoma (MCF 7) cells. Hence, it is suggested that Dox NP ?+?Ver NP is a promising administration for tumor therapy.
机译:多药耐药性(MDR)是肿瘤细胞治疗反应不足的最常见问题。已经开发出许多试验来克服P-糖蛋白(P-GP)的药物流出。例如,共同给予许多药物,称为化学敏胶剂或MDR调节剂,具有化学治疗剂以抑制药物流出。但是对于最佳协同作用,药物和抑制剂组合可能需要在肿瘤细胞中在时间上逐渐分析。在这项研究中,我们将Ver和Dox封装在PLGA纳米粒子中以抑制乳腺癌的P-GP药物流出。此外,DOX溶液(DOX S),DOX纳米粒子(DOX NP),DOX S?+?ver s,dox np?ver s,dox np?+?ver np或dox-ver np的影响。发现具有Ver NP(70.76%)的DOX NP的CO施用与DOX / VER组合溶液(70.62%)显示出类似的蜂窝状摄取。然而,观察到DOX NP?+?Ver NP具有最高的凋亡活动(早期凋亡13.52?±0.06%,晚期凋亡53.94?±0.15%)在人乳腺腺癌(MCF 7)细胞上。因此,建议Dox NP?+?Ver NP是肿瘤治疗的有希望的给药。

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