首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >Poly(ethylene glycol)-radix Ophiopogonis polysaccharide conjugates: preparation, characterization, pharmacokinetics and in vitro bioactivity.
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Poly(ethylene glycol)-radix Ophiopogonis polysaccharide conjugates: preparation, characterization, pharmacokinetics and in vitro bioactivity.

机译:聚乙二醇基麦冬多糖共轭物:制备,表征,药代动力学和体外生物活性。

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摘要

Radix Ophiopogonis polysaccharide (ROP), a natural graminan-type fructan with Mw of approximately 5kDa, had been found to have an excellent anti-myocardial ischemic activity. However, its rapid renal excretion following administration remarkably limits its efficacy and clinical use, which makes necessary the development of an effective delivery system. In this article, the feasibility of PEGylation to solve this problem was examined. A moderate coupling reaction between the hydroxyl-activated ROP and the amino-terminated mPEG was chosen to PEGylate ROP. Five different mPEG-ROP conjugates (with mPEG of molecular mass 2, 5 or 20kDa) were prepared, purified, characterized and evaluated in pharmacokinetics and in vitro bioactivity. Results showed that only when the apparent molecular weight of the conjugate approached to a certain value, would its plasma elimination reduce abruptly. In general, the conjugation caused the reduction in the bioactivity of ROP; however, well-preserved bioactivity was observed when the grafting degree of the conjugate was lower. Among the five conjugates studied, the one with an average 1.3 mPEG (20kDa) residues per single ROP was found to be satisfactory both in plasma retention and in bioactivity. It had a 47.4-fold increased elimination half-life and preserved approximately 74% of the bioactivity of ROP; moreover, the decrease in bioactivity is not significant. These findings demonstrate that PEGylation would be a promising approach for improving the clinical efficacy of ROP by prolonged retention in plasma.
机译:麦冬多糖(ROP)是一种天然的格拉米聚糖型果聚糖,其Mw约为5kDa,具有出色的抗心肌缺血活性。但是,给药后其快速的肾脏排泄明显限制了它的功效和临床应用,这使得必须开发有效的递送系统。在本文中,研究了PEG化解决此问题的可行性。选择羟基活化的ROP和氨基封端的mPEG之间的中等偶联反应以使ROP聚乙二醇化。制备,纯化,表征和评估了五种不同的mPEG-ROP缀合物(分子量分别为2、5或20kDa的mPEG),药代动力学和体外生物活性。结果表明,只有当缀合物的表观分子量达到一定值时,其血浆消除才会突然减少。通常,缀合导致ROP的生物活性降低;然而,当缀合物的接枝度较低时,观察到保存良好的生物活性。在研究的五种缀合物中,发现每个单ROP平均残基为1.3 mPEG(20kDa)的缀合物在血浆保留和生物活性方面均令人满意。它的消除半衰期延长了47.4倍,并保留了ROP约74%的生物活性。此外,生物活性的降低并不明显。这些发现表明,聚乙二醇化将是通过延长在血浆中保留时间来提高ROP临床疗效的一种有前途的方法。

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