生物分析
药物开发
计算生物学
模式
药品
制药工业
药理学
化学
生物
色谱法
社会科学
社会学
作者
Amanda Hays,Mark Wissel,Kelly Colletti,Russell K. Soon,Mitra Azadeh,Justin S. Smith,Rajitha Doddareddy,Melanie Chalfant,Wendy O. Adamowicz,Swarna Suba Ramaswamy,Sanjay L. Dholakiya,Sebastián Guelman,Bryan Gullick,Jennifer N. Durham,Keith Rennier,Pruthvi Nagilla,Anamica Muruganandham,Manisha R. Diaz,Cassandra A. Tierney,Kaarthik John
出处
期刊:Aaps Journal
[Springer Science+Business Media]
日期:2024-02-05
卷期号:26 (1): 24-24
被引量:22
标识
DOI:10.1208/s12248-023-00880-9
摘要
Abstract The emerging use of qPCR and dPCR in regulated bioanalysis and absence of regulatory guidance on assay validations for these platforms has resulted in discussions on lack of harmonization on assay design and appropriate acceptance criteria for these assays. Both qPCR and dPCR are extensively used to answer bioanalytical questions for novel modalities such as cell and gene therapies. Following cross-industry conversations on the lack of information and guidelines for these assays, an American Association of Pharmaceutical Scientists working group was formed to address these gaps by bringing together 37 industry experts from 24 organizations to discuss best practices to gain a better understanding in the industry and facilitate filings to health authorities. Herein, this team provides considerations on assay design, development, and validation testing for PCR assays that are used in cell and gene therapies including (1) biodistribution; (2) transgene expression; (3) viral shedding; (4) and persistence or cellular kinetics of cell therapies. Graphical Abstract
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