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A humanized monoclonal antibody targeting secreted anterior gradient 2 effectively inhibits the xenograft tumor growth

人源化抗体 免疫原性 单克隆抗体 抗体 表位 癌症研究 生物 癌症 分子生物学 计算生物学 化学 免疫学 遗传学
作者
Hao Guo,Hao Chen,Qi Zhu,Xiaoyan Yu,Rong Rong,Siva Bharath Merugu,Hitesh Bhagavanbhai Mangukiya,Dawei Li
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier BV]
卷期号:475 (1): 57-63 被引量:23
标识
DOI:10.1016/j.bbrc.2016.05.033
摘要

Anterior Gradient 2 (AGR2) is a potential anti-tumor target and we previously reported a murine antibody 18A4 with specific binding to AGR2. However, humanization is a must to overcome immunogenicity before considering for clinical use and optimized vectors for mammalian expression are also necessary for following industrialized manufacture. Here, we describe an anti-tumor humanized antibody blocking secreted AGR2 activity. We employed the CDR grafting technique and deimmunization analysis to construct humanized antibody variants of 18A4, and 18A4Hu I was selected as the best humanization candidate, characterized by physical and chemical property comparison. Mouse xenograft study showed that 18A4Hu I could effectively inhibit the xenograft tumor growth, antibody blocking epitope analysis using AGR2 mutants indicated that the inhibition activity of 18A4Hu I is exerted probably through blocking the AGR2 functions which rely on the amino acid sites of E60-H76 and A86-E153. What’s more, in this report, we also describe a pHAb-FAST vector system which is specifically designed for humanized antibody mammalian expression vector fast construction. With pHAb-FAST system, expression vector of 18A4Hu I could be quickly constructed only through twice overlapping PCR reactions. To our knowledge, AGR2-targeted 18A4Hu I is a promising humanized anti-tumor drug candidate, and pHAb-FAST system is a useful optimized mammalian expression vector construction tool. Our findings are supposed to accelerate the development of antibody-based cancer therapy.
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