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The application of EDTA in drug delivery systems: doxorubicin liposomes loaded via NH4EDTA gradient

机译:EDTA在药物递送系统中的应用:通过NH4EDTA梯度加载的阿霉素脂质体

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摘要

The applications of ethylenediaminetetraacetic acid (EDTA) have been expanded from the treatment of heavy metal poisoning to chelation therapies for atherosclerosis, heart disease, and cancers, in which EDTA reduces morbidity and mortality by chelating toxic metal ions. In this study, EDTA was used in a drug delivery system by adopting an NH4EDTA gradient method to load doxorubicin into liposomes with the goal of increasing therapeutic effects and decreasing drug-related cytotoxicity. The particle size of the optimum NH4EDTA gradient liposomes was 79.4±1.87 nm, and the entrapment efficiency was 95.54%±0.59%. In vitro studies revealed that liposomes prepared using an NH4EDTA gradient possessed long-term stability and delayed drug release. The in vivo studies also showed the superiority of the new doxorubicin formulation. Compared with an equivalent drug dose (5 mg/kg) prepared by (NH4)2SO4 gradient, NH4EDTA gradient liposomes showed no significant differences in tumor inhibition ratio, but cardiotoxicity and liposome-related immune organ damage were lower, and no drug-related deaths were observed. These results show that use of the NH4EDTA gradient method to load doxorubicin into liposomes could significantly reduce drug toxicity without influencing antitumor activity.
机译:乙二胺四乙酸(EDTA)的应用已从重金属中毒的治疗扩展到用于动脉粥样硬化,心脏病和癌症的螯合疗法,其中EDTA通过螯合有毒金属离子来降低发病率和死亡率。在这项研究中,EDTA通过采用NH4EDTA梯度法将阿霉素加载到脂质体中而用于药物递送系统,目的是提高治疗效果并降低药物相关的细胞毒性。最佳NH4EDTA梯度脂质体的粒径为79.4±1.87 nm,包封率为95.54%±0.59%。体外研究表明,使用NH4EDTA梯度制备的脂质体具有长期稳定性和延迟的药物释放。体内研究还显示了新的阿霉素制剂的优越性。与通过(NH4)2SO4梯度制备的当量药物剂量(5 mg / kg)相比,NH4EDTA梯度脂质体在肿瘤抑制率上没有显着差异,但是心脏毒性和脂质体相关的免疫器官损害较低,并且没有药物相关的死亡被观察。这些结果表明,使用NH4EDTA梯度法将阿霉素加载到脂质体中可以显着降低药物毒性而不影响抗肿瘤活性。

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