粘度
赋形剂
生化工程
药品
药物开发
化学
纳米技术
材料科学
热力学
药理学
色谱法
医学
物理
工程类
作者
Dheeraj S. Tomar,Sandeep Kumar,Satish Kumar Singh,Sumit Goswami,Li Li
出处
期刊:mAbs
[Landes Bioscience]
日期:2016-01-06
卷期号:8 (2): 216-228
被引量:196
标识
DOI:10.1080/19420862.2015.1128606
摘要
Effective translation of breakthrough discoveries into innovative products in the clinic requires proactive mitigation or elimination of several drug development challenges. These challenges can vary depending upon the type of drug molecule. In the case of therapeutic antibody candidates, a commonly encountered challenge is high viscosity of the concentrated antibody solutions. Concentration-dependent viscosity behaviors of mAbs and other biologic entities may depend on pairwise and higher-order intermolecular interactions, non-native aggregation, and concentration-dependent fluctuations of various antibody regions. This article reviews our current understanding of molecular origins of viscosity behaviors of antibody solutions. We discuss general strategies and guidelines to select low viscosity candidates or optimize lead candidates for lower viscosity at early drug discovery stages. Moreover, strategies for formulation optimization and excipient design are also presented for candidates already in advanced product development stages. Potential future directions for research in this field are also explored.
科研通智能强力驱动
Strongly Powered by AbleSci AI