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Assessment of DNA damage in Ehlrich carcinoma after treatment with doxorubicin encapsulated in nanoscales thermosensitive liposomes in combination with localized hyperthermia

机译:纳米级热敏脂质体中封装的阿霉素联合局部热疗后评估Ehlrich癌的DNA损伤

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Nanoscales thermosensitive liposomes (TSL) composed of synthetic lipids (dipalmitoyl-phosphatidylcholine, and distearoylphosphatidylcholine), were used for doxorubicin encapsulation with 70% encapsulated efficiency. The liposomes were characterized by dynamic light scattering, transmission electron microscopy and turbidity method. Additionally, the liposomes exhibited a significant release of doxorubicin (Dox) by 60% within 5 min at 42 degrees C. To assess the therapeutic efficacy of Dox in combination with hyperthermia, Dox free and encapsulated TSL were administered directly to Ehrlich tumor bearing mice at 1 mg/kg dose. Immediately after the drug administration, hyperthermia was applied to mention the temperature inside the tumor site at 42 degrees C either for 5 min and 30 min. The results indicate a significant increase in the percent of apoptotic and necrotic cells in the treated group. Moreover, disrupts the integrity and the amount of intact DNA in tumor cells. In conclusion, Dox and hyperthermia may serve as a useful targeted drug delivery system for management of Ehrlich carcinoma.
机译:由合成脂质(二棕榈酰磷脂酰胆碱和二硬脂酰磷脂酰胆碱)组成的纳米级热敏脂质体(TSL)用于阿霉素的封装,封装效率为70%。通过动态光散射,透射电子显微镜和浊度法对脂质体进行了表征。另外,脂质体在42摄氏度下5分钟内显示出60%的阿霉素(Dox)显着释放。为了评估Dox与热疗结合的治疗效果,将无Dox的和包囊的TSL直接施用于Ehrlich肿瘤小鼠1 mg / kg剂量。药物给药后,立即进行热疗以提及42℃下肿瘤部位内部的温度5分钟和30分钟。结果表明,治疗组中凋亡和坏死细胞的百分比显着增加。而且,破坏了肿瘤细胞中完整性和完整DNA的量。总之,Dox和热疗可以作为治疗艾氏癌的有用靶向药物递送系统。

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