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Targeted Therapy for Hepatocellular Carcinoma: Co-Delivery of Sorafenib and Curcumin Using Lactosylated pH-Responsive Nanoparticles

机译:用于肝细胞癌的靶向治疗:使用乳糖基化的pH-响应纳米颗粒共同递送Sorafenib和姜黄素

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Purpose: Hepatocellular carcinoma (HCC) is a leading cancer worldwide. In the present investigation, sorafenib (SFN) and curcumin (CCM) were co-delivered using pH-sensitive lactosylated nanoparticles (LAC-NPs) for targeted HCC treatment. Methods: pH-responsive lactosylated materials were synthesized. SFN and CCM co-delivered, pH-responsive lactosylated nanoparticles (LAC-SFN/CCM-NPs) were self-assembled by using the nanoprecipitation technique. The nanoparticles were characterized in terms of particle size, charge and drug release profile. The anti-cancer effects of the nanoparticles were evaluated in human hepatic carcinoma cells (HepG2) cells and HCC tumor xenograft models. Results: LAC-SFN/CCM-NPs are spherical particles with light coats on the surface. The size and zeta potential of LAC-SFN/CCM-NPs were 115.5 ± 3.6 nm and ? 34.6 ± 2.4, respectively. The drug release of LAC-SFN/CCM-NPs in pH 5.5 was more efficient than in pH 7.4. LAC-SFN/CCM-NPs group exhibited the smallest tumor volume (239 ± 14 mmsup3/sup), and the inhibition rate of LAC-SFN/CCM-NPs was 77.4%. Conclusion: In summary, LAC-SFN/CCM-NPs was proved to be a promising system for targeted HCC therapy.
机译:目的:肝细胞癌(HCC)是全世界领先的癌症。在本发明的研究中,使用pH敏感的乳糖基化的纳米颗粒(LAC-NPS)共同递送Sorafenib(SFN)和姜黄素(CCM),用于靶向HCC处理。方法:合成pH-响应乳糖基化材料。通过使用纳米沉淀技术,通过使用纳米沉淀技术自组装SFN和CCM共递送的pH-响应乳糜囊化纳米颗粒(LAC-SFN / CCM-NPS)。纳米颗粒的特征在于粒度,电荷和药物释放型材。在人肝癌细胞(HEPG2)细胞和HCC肿瘤异种移植模型中评价纳米颗粒的抗癌作用。结果:LAC-SFN / CCM-NPS是具有光涂层的球形颗粒。 LAC-SFN / CCM-NPS的尺寸和Zeta电位为115.5±3.6nm和? 34.6±2.4分别。 LAC-SFN / CCM-NPS在pH 5.5中的药物释放比pH7.4更有效。 LAC-SFN / CCM-NPS组显示出最小的肿瘤体积(239±14 mm 3 ),LAC-SFN / CCM-NP的抑制率为77.4%。结论:总之,LAC-SFN / CCM-NPS被证明是靶向HCC疗法的有希望的系统。

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