生物仿制药
生物分析
药代动力学
许可证
药理学
医学
化学
计算机科学
内科学
色谱法
操作系统
作者
Dana T Hackel,Theingi M. Thway,Shiew Mei Huang,Yow‐Ming Wang
出处
期刊:Bioanalysis
[Newlands Press Ltd]
日期:2021-09-01
卷期号:13 (17): 1323-1332
被引量:4
标识
DOI:10.4155/bio-2021-0116
摘要
The presence of circulating targets and antidrug antibodies can influence the ability of a bioanalytical method to measure therapeutic protein (TP) concentration relevant to exposure-response evaluations. This project surveyed biosimilar submissions for their bioanalytical methods. Survey results revealed that 97% of pharmacokinetic methods designed to measure theoretically free or partial-free TPs with respect to target indeed measured free or partial-free TPs when considering experimental testing results for target effects. Antidrug antibody effect is less often evaluated. The observed trend of measuring biologically active forms of TP is consistent with the scientific understanding that pharmacokinetics of biologically active forms is more likely to be relevant to the clinical responses and evaluation of clinically meaningful differences to contribute to biosimilarity assessments.
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