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Enhanced antitumor efficacy on hepatoma-bearing rats with adriamycin-loaded nanoparticles administered into hepatic artery

机译:负载阿霉素纳米颗粒的肝癌大鼠对肝癌大鼠的抗肿瘤功效增强

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摘要

AIM: To investigate the antitumor activity of adriamycin (ADR) encapsulated in nanoparticles (NADR) and injected into the hepatic artery of hepatoma-bearing rats.METHODS: NADR was prepared by the interfacial polymerization method. Walker-256 carcinosarcomas were surgically implanted into the left liver lobes of 60 male Wistar rats, which were divided into 4 groups at random (15 rats per group). On the 7th day after implantation, normal saline (NS), free ADR (FADR), NADR, or ADR mixed with unloaded nanoparticles (ADR + NP) was respectively injected via the hepatic artery (i.a.) of rats in different groups. The dose of ADR in each formulation was 2.0 mg/kg body weight and the concentration was 1.0 mg/mL. Survival time, tumor enlargement ratio, and tumor necrosis degree were compared between each group.RESULTS: Compared with the rats that received NS i.a., the rats that received FADR or ADR + NP acquired apparent inhibition on tumor growth, as well as prolonged their life span. Further significant anticancer efficacy was observed in rats that received i.a. administration of NADR. Statistics indicated that NADR brought on a more significant tumor inhibition and more extensive tumor necrosis, as compared to FADR or ADR + NP. The mean tumor enlargement ratio on the 7th day after NADR i.a. was 1.106. The mean tumor-bearing survival time was 39.50 days. Prolonged life span ratio was 109.22% as compared with rats that accepted NS.CONCLUSION: Therapeutic effect of ADR on liver malignancy can be significantly enhanced by its nanopaticle formulation and administration via hepatic artery.
机译:目的:研究包裹在纳米颗粒(NADR)中并注入荷瘤大鼠肝动脉中的阿霉素(ADR)的抗肿瘤活性。方法:采用界面聚合法制备NADR。将Walker-256癌肉瘤通过手术植入60只雄性Wistar大鼠的左肝叶中,随机分为4组(每组15只大鼠)。植入后第7天,分别通过不同组大鼠的肝动脉(i.a.)注射生理盐水(NS),游离ADR(FADR),NADR或与未负载纳米颗粒(ADR + NP)混合的ADR。每种制剂中的ADR剂量为2.0 mg / kg体重,浓度为1.0 mg / mL。结果:与接受NS ia的大鼠相比,接受FADR或ADR + NP的大鼠对肿瘤的生长有明显的抑制作用,并延长了它们的寿命,从而比较了两组的存活时间,肿瘤扩大率和肿瘤坏死程度。跨度。在接受i.a.的大鼠中观察到进一步显着的抗癌功效。 NADR的管理。统计数据表明,与FADR或ADR + NP相比,NADR带来了更显着的肿瘤抑制和更广泛的肿瘤坏死。 NADR后第7天的平均肿瘤扩大率是1.106。平均荷瘤生存时间为39.50天。结论:ADR的纳米粒配方和通过肝动脉给药可显着增强ADR对肝恶性肿瘤的治疗作用。

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