Bioanalytical Services Department, WuXi AppTec, 288 Fute Zhong Road, Waigaoqiao, Shanghai, 200131, China.
AAPS J. 2021 May 3;23(3):64. doi: 10.1208/s12248-021-00594-w.
In the absence of regulatory guidelines for the bioanalysis of new drug modalities, many of which contain multiple functional domains, bioanalytical strategies have been carefully designed to characterize the intact drug and each functional domain in terms of quantity, functionality, biotransformation, and immunogenicity. The present review focuses on the bioanalytical challenges and considerations for RNA-based drugs, bispecific antibodies and multi-domain protein therapeutics, prodrugs, gene and cell therapies, and fusion proteins. Methods ranging from the conventional ligand binding assays and liquid chromatography-mass spectrometry assays to quantitative polymerase chain reaction or flow cytometry often used for oligonucleotides and cell and gene therapies are discussed. Best practices for method selection and validation are proposed as well as a future perspective to address the bioanalytical needs of complex modalities.
在缺乏新药物模式的生物分析监管指南的情况下,其中许多药物包含多个功能域,因此精心设计了生物分析策略,以从数量、功能、生物转化和免疫原性方面来描述完整药物和每个功能域。本综述重点介绍了基于 RNA 的药物、双特异性抗体和多结构域蛋白治疗药物、前药、基因和细胞治疗以及融合蛋白的生物分析挑战和注意事项。讨论了常用于寡核苷酸和细胞及基因治疗的方法,包括传统的配体结合测定法和液相色谱-质谱联用法,以及定量聚合酶链反应或流式细胞术。还提出了方法选择和验证的最佳实践,以及解决复杂模式的生物分析需求的未来展望。
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