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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Enhanced pharmacological activity of recombinant human interleukin-11 (rhIL11) by chemical modification with polyethylene glycol
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Enhanced pharmacological activity of recombinant human interleukin-11 (rhIL11) by chemical modification with polyethylene glycol

机译:通过聚乙二醇化学修饰增强重组人白介素11(rhIL11)的药理活性

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摘要

In order to improve the pharmacological efficacy of recombinant human interleukin-11 (rhIL11) and to reduce the frequency of administration, we examined the feasibility of chemical modification of rhIL11 by polyethylene glycol. The rhIL11 was chemically modified by using branched type (PEG2), or linear type (PEG) polyethylene glycol-N-hydroxysuccinimide with various molecular weights. Plasma profiles of immunoreactive rhIL11 after i.v. injection of the 20 kDa PEG2 conjugated rhIL11 (PEG2 (20 K)-rhIL11) were determined by ELISA. Peripheral platelet counts after the administration of the various conjugates were measured. Pharmacokinetic analysis revealed that the mean residence time of PEG2 (20 K)-rhIL11 after i.v. injection extensively increased by a factor of ca 60 compared with the native rhIL11. Maximum peripheral platelet increase of 67% for PEG2 (20 K)-rhIL11 and that of 50% for PEG (20 K)-rhIL11 over the control was observed whereas no significant change was associated with the bolus i.v. injection of native rhIL11. On the other hand, the remaining biological activity of these PEGylated-rhIL11s was 14–16% of native rhIL11, suggesting that retention of rhIL11 in plasma is much effective in order to potentiate the pharmacological efficacy of the cytokine. Chemical modification of rhIL11 by PEG is a promising approach for improving the clinical efficacy of rhIL11 by prolonged retention in plasma.
机译:为了提高重组人白介素11(rhIL11)的药理功效并减少给药频率,我们研究了用聚乙二醇化学修饰rhIL11的可行性。通过使用具有各种分子量的支链型(PEG2)或线性型(PEG)聚乙二醇-N-羟基琥珀酰亚胺对rhIL11进行化学修饰。静脉注射后免疫反应性rhIL11的血浆特征通过ELISA确定20kDa PEG2缀合的rhIL11(PEG2(20K)-rhIL11)的注射。在施用各种缀合物后测量外周血小板计数。药代动力学分析表明,经静脉内注射后,PEG2(20 K)-rhIL11的平均停留时间。与天然rhIL11相比,注射剂量可增加约60倍。观察到与对照相比,PEG2(20 K)-rhIL11的最大外周血血小板增加了67%,而PEG(20 K)-rhIL11的最大外周血血小板增加了50%,而推注i.v没有明显变化。注射天然rhIL11。另一方面,这些聚乙二醇化的rhIL11s的剩余生物学活性是天然rhIL11的14–16%,这表明rhIL11在血浆中的保留对于增强细胞因子的药理效力非常有效。通过PEG对rhIL11进行化学修饰是通过延长在血浆中的保留来提高rhIL11的临床疗效的一种有前途的方法。

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