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首页> 外文期刊>Die Pharmazie >Pharmacokinetics of rh-IFNalpha-2a-NGR, a tumor targeted-therapy candidate, following intramuscular administration to mice, rats and monkeys.
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Pharmacokinetics of rh-IFNalpha-2a-NGR, a tumor targeted-therapy candidate, following intramuscular administration to mice, rats and monkeys.

机译:向小鼠,大鼠和猴子肌肉内给药后,rh-IFNalpha-2a-NGR(一种肿瘤靶向治疗药物)的药代动力学。

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摘要

The compound rh-IFNalpha-2a-NGR can inhibit tumor angiogenesis and could be used for targeted therapy. In the present study, double antibody sandwich ELISA analysis was used to determine the concentration of rh-IFNalpha-2a-NGR in serum after intramuscular administration of various dosages to mice, rats and monkeys. The results showed that the pharmacokinetic properties of rh-IFNalpha2a-NGR after i.m. administration to mice, rats and monkeys were consistent with a one-compartment open model. The main pharmacokinetic parameters in mice (9.36 microg/kg), rats (4.68 microg/kg) and monkeys (2.34 microg/kg) after i.m. rh-IFNalpha2a-NGR were as follows: T(peak) was 0.49, 1.65 and 3.60h, C(max) was 3030.20, 654.49 and 268.13 ng/L, t1/2 was 0.39, 4.52 and 2.70 h, and AUC(0-infinity)) was 4197.65, 5784.58 and 2622.06 ng/L x h, respectively. Also, mice, rats and monkeys had their own distinct metabolic characteristics. These data would provide references for further clinical pharmacokinetic study of rh-IFNalpha2a-NGR.
机译:化合物rh-IFNalpha-2a-NGR可抑制肿瘤血管生成,可用于靶向治疗。在本研究中,使用双重抗体夹心ELISA分析来确定在向小鼠,大鼠和猴子肌肉内施用各种剂量后血清中rh-IFNalpha-2a-NGR的浓度。结果表明,r.IFNα2a-NGR在i.m后的药代动力学特性。对小鼠,大鼠和猴子的给药与一室开放模型一致。 i.m.后小鼠(9.36 microg / kg),大鼠(4.68 microg / kg)和猴子(2.34 microg / kg)的主要药代动力学参数。 rh-IFNalpha2a-NGR如下:T(peak)为0.49、1.65和3.60h,C(max)为3030.20、654.49和268.13 ng / L,t1 / 2为0.39、4.52和2.70 h,以及AUC(0 -无穷大)分别为4197.65、5784.58和2622.06 ng / L xh。而且,小鼠,大鼠和猴子具有自己独特的代谢特征。这些数据将为rh-IFNalpha2a-NGR的进一步临床药代动力学研究提供参考。

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