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重组人促红细胞生成素-Fc融合蛋白的体内药代动力学和药效学

Pharmacokinetics and pharmacodynamics of recombinant human EPO-Fc fusion protein in vivo.

作者信息

Shi Xunlong, Yang Jianjun, Zhu Haiyan, Ye Li, Feng Meiqing, Li Jiyang, Huang Hai, Tao Qun, Ye Dan, Sun Lee-Hwei K, Sun Bill N C, Sun Cecily R Y, Han Guizhen, Liu Yuanyuan, Yao Minghui, Zhou Pei, Ju Dianwen

机构信息

Department of Biosynthesis, School of Pharmacy, Fudan University, Shanghai, China.

出版信息

PLoS One. 2013 Aug 19;8(8):e72673. doi: 10.1371/journal.pone.0072673. eCollection 2013.

Abstract

In this study, the in vivo pharmacokinetics and pharmacodynamics of a novel recombinant human erythropoietin (rhEPO) Fc fusion protein, rhEPO-Fc, were studied in both rodents and rhesus monkeys. Animal models of anemia induced by irradiation, cyclophosphamide and partial renal ablation were used to evaluate therapeutic effects of rhEPO-Fc. We have demonstrated that serum half-life of rhEPO-Fc was 29.5 to 38.9 h at doses of 8, 25, 80 µg/kg in rhesus monkeys and 35.5 to 43.5 h at doses of 16, 50, 160 µg/kg in rats. In anemia animal models, rhEPO-Fc dose-dependently (7.5-30.0 µg/kg in mice, 5.4-21.4 µg/kg in rats and 5.0-10.0 µg/kg in rhesus monkeys) increased reticulocyte level, followed by an increase of RBC count, hemoglobin and hematocrit levels. At reduced intervention frequency of weekly treatments, rhEPO-Fc showed similar hematopoietic effects as compared with rhEPO given three times a week. These results indicated that rhEPO-Fc could potentially be used in treatment of anemia and warrants future clinical trials.

摘要

在本研究中,对一种新型重组人促红细胞生成素(rhEPO)Fc融合蛋白rhEPO-Fc在啮齿动物和恒河猴体内的药代动力学和药效学进行了研究。采用辐射、环磷酰胺和部分肾切除诱导的贫血动物模型来评估rhEPO-Fc的治疗效果。我们已证明,在恒河猴中,rhEPO-Fc剂量为8、25、80μg/kg时血清半衰期为29.5至38.9小时,在大鼠中剂量为16、50、160μg/kg时血清半衰期为35.5至43.5小时。在贫血动物模型中,rhEPO-Fc剂量依赖性地(小鼠为7.5 - 30.0μg/kg,大鼠为5.4 - 21.4μg/kg,恒河猴为5.0 - 10.0μg/kg)提高网织红细胞水平,随后红细胞计数、血红蛋白和血细胞比容水平升高。在每周治疗干预频率降低的情况下,rhEPO-Fc与每周给药三次的rhEPO相比显示出相似的造血作用。这些结果表明,rhEPO-Fc有可能用于治疗贫血,值得进行未来的临床试验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a4bd/3747110/26864822becc/pone.0072673.g001.jpg

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