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In vivo performance of implantable biodegradable preparations delivering Paclitaxel and Etanidazole for the treatment of glioma.

机译:递送紫杉醇和依替硝唑的可植入生物可降解制剂的体内性能用于治疗神经胶质瘤。

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摘要

Drug-releasing implants delivering chemotherapeutic and radio-sensitizing agents are beginning to play a major role in the post-surgical eradication of residual glioma in the brain. Benefits from early arresting of tumor growth and tumor recovery dynamics stress the impact of drug release profiles of the implants on the efficacy of the treatment. This paper examines responses of BALB/c nude mice, bearing C6 glioma tumors subcutaneously, to treatments by PLGA microspheres, microparticles and discs-delivering Paclitaxel and Etanidazole. The experimental results are used to correlate the efficacy of treatment to in vitro release profiles from the various formulations. Our study demonstrates that radio-sensitizing effects during irradiation could be achieved by double burst profiles from Etanidazole-loaded discs, when compared to controls 17 days after implantation despite the short half-life of Etanidazole (1.4h) in vivo. These results also showed inhibited tumor growth on tumor volumes of 59%, 65% and 70% over the blank placebo groups after 21 days of tumor growth for spray-dried microspheres, electrohydrodynamic atomization microparticles and spray-dried discs, respectively.
机译:释放释放药物的化学治疗剂和放射增敏剂开始在脑部残余神经胶质瘤的手术后根除中起主要作用。早期阻止肿瘤生长和肿瘤恢复动力学的好处强调了植入物的药物释放曲线对治疗功效的影响。本文研究了皮下带有C6胶质瘤肿瘤的BALB / c裸鼠对PLGA微球,微粒和碟形紫杉醇和依替硝唑治疗的反应。实验结果用于将治疗功效与各种制剂的体外释放曲线相关联。我们的研究表明,尽管在体内植入Etanidazole的半衰期很短(1.4h),但与植入后17天的对照组相比,通过装载Etanidazole的椎间盘进行两次爆破可以实现辐射期间的放射增敏作用。这些结果还表明,在21天的肿瘤生长后,对于喷雾干燥的微球,电动流体雾化微粒和喷雾干燥的椎间盘,空白对照组的肿瘤生长受到抑制,其肿瘤体积分别为59%,65%和70%。

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