体内分布
聚乙二醇化
PEG比率
聚乙二醇
化学
药代动力学
细胞内
生物化学
药理学
分布(数学)
生物分析
生物物理学
生物
体外
色谱法
财务
数学分析
经济
数学
作者
Andreas Baumann,Dietrich Tuerck,Saileta Prabhu,Leslie J. Dickmann,Jennifer Sims
标识
DOI:10.1016/j.drudis.2014.06.002
摘要
The pharmacokinetics (PK), metabolism and biodistribution of polyethylene glycol (PEG) in PEGylated proteins are important to understand the increased cellular vacuolation reported in various tissues in animals. The tissue distribution profile of PEGylated proteins and 'metabolic' PEG is guided largely by absolute PEG load, PEG molecular weight and, where applicable, receptor-mediated uptake via the protein moiety. High molecular weight PEGs show slow renal clearance, and consequently have a greater potential to accumulate within cells. The intracellular nonbiodegradable PEG can accumulate within the lysosome ultimately causing distension and vacuolation observed by standard histological examinations. Improved bioanalytical methodologies will contribute to the identification of specific PK parameters including distribution behavior to support development of PEGylated proteins as therapeutics.
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