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首页> 外文期刊>Journal of materials science >In vivo investigation of ceftiofur-loaded gelatin and PLGA microspheres in beagle dogs
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In vivo investigation of ceftiofur-loaded gelatin and PLGA microspheres in beagle dogs

机译:比格犬体内头孢噻呋明胶和PLGA微球的体内研究

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摘要

Drug delivery systems based on polymer microspheres have received considerable attention. Cef-tiofur sodium and ceftiofur hydrochloride is widely used for the treatment of bacterial diseases in animals but the delivery in vivo has not been reported. In this paper, we report the synthesis of microspheres from gelatin and PLGA, two kinds of typical natural and artificial materials, for loading ceftiofur and the in vivo investigation of the pharmacokinetics in beagle dogs. By controlling the synthesis parameters, gelatin and PLGA microspheres with diameter between 5 and 35 microns were obtained. Assay procedures based on high performance liquid chromatog-raphy were evaluated and confirmed. The dogs were randomly divided into three groups, i.e., control group, gelatin group, and PLGA group and administrated via intravenous injection. Plasma concentrations of ceftiofur over time were measured and analyzed. Results indicate that the main kinetic parameters do not show significant difference for the gelatin group and control group, but the area under the curve, plasma half-life, apparent volume of distribution, and clearance ratio of PLGA group show significant difference from the gelatin group and the control group. The PLGA microspheres show a low area under the curve but long time release.
机译:基于聚合物微球的药物递送系统已受到相当大的关注。头孢噻呋钠和头孢噻呋盐酸盐被广泛用于治疗动物细菌性疾病,但尚未报道体内递送。在本文中,我们报道了由明胶和PLGA(两种典型的天然和人工材料)合成的微球,用于负载头孢噻呋和体内研究比格犬的药代动力学。通过控制合成参数,获得了直径在5到35微米之间的明胶和PLGA微球。对基于高效液相色谱的测定程序进行了评估和确认。将狗随机分为三组,即对照组,明胶组和PLGA组,并通过静脉内注射给药。测量并分析了头孢噻呋随时间的血浆浓度。结果表明,明胶组和对照组的主要动力学参数无明显差异,但曲线下面积,血浆半衰期,表观分布体积和清除率与明胶组相比有显着差异。和对照组。 PLGA微球在曲线下的面积较小,但释放时间较长。

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  • 来源
    《Journal of materials science 》 |2013年第4期| 903-910| 共8页
  • 作者单位

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Qingdao KDN Animal Drugs Technology Development Research Center, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

    Laboratories of Biological Pharmaceutical, College of Chemical and Pharmaceutical Sciences, Qingdao Agricultural University, Qingdao 266061, China;

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