Biosimilars and biobetters as tools for understanding and mitigating the immunogenicity of biotherapeutics

被引:16
|
作者
Barbosa, Maria D. F. S. [1 ]
Kumar, Sandeep [2 ]
Loughrey, Helen
Singh, Satish K. [2 ]
机构
[1] Bristol Myers Squibb Co, Bioanalyt Sci, Princeton, NJ 08543 USA
[2] Pfizer Inc, Biotherapeut Pharmaceut Sci, Chesterfield, MO 63017 USA
关键词
AGGREGATION-PRONE REGIONS; HUMAN INTERFERON-BETA; THERAPEUTIC PROTEINS; NEUTRALIZING ANTIBODIES; BIOTECHNOLOGY PRODUCTS; SEQUENCE DETERMINANTS; INSULIN GLARGINE; HOST ANTIBODIES; HEMOPHILIA-A; IFN-BETA;
D O I
10.1016/j.drudis.2012.07.003
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
In this article, we review key steps for the development of biosimilars and biobetters and related bioanalytical challenges, with a focus on how they are associated with immunogenicity. We analyze the factors that can impact antidrug antibody (ADA) responses and their correlations with preclinical and clinical outcomes to provide relevant insights and to answer questions, including what types of aggregate are immunogenic. We also address strategies for developing less-immunogenic biotherapeutics. Using interferon-beta (IFN-beta) as a case study, we explore the correlation between aggregation and immunogenicity. We dissect and integrate with clinical data the IFN-beta preclinical immunogenicity and aggregation predictions and discuss the feasibility of developing an IFN-beta with lower aggregation and/or immunogenicity.
引用
收藏
页码:1282 / 1288
页数:7
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