A Novel Anti-EGFR mAb Ame55 with Lower Toxicity and Better Efficacy than Cetuximab When Combined with Irinotecan.

Weiyi QiuChang ZhangShuang WangXiaoyan YuQiong WangDadi ZengPeng DuJinling MaYiqiong ZhengBo PangYunzhou YuFeng LongXiaobin Pang Zhiwei Sun

Published in: Journal of immunology research (2019)

To improve efficacy and minimize toxicity of EGFR inhibition treatment, we developed Ame55, a novel anti-EGFR IgG1 with lower affinity to EGFR than cetuximab (C225) from a human phage library. Ame55 had lower bioactivity than cetuximab in vitro but similar antitumor efficacy as cetuximab in vivo. Moreover, Ame55 was more efficacious than cetuximab in a Lovo cell xenograft tumor model when combined with irinotecan (CPT-11). Ame55 concentrates in the mouse xenograft tumor and has less toxicity than cetuximab in cynomolgus monkeys in an overdose study.

Keyphrases

metastatic colorectal cancer
small cell lung cancer
epidermal growth factor receptor
locally advanced
wild type
tyrosine kinase
oxidative stress
endothelial cells
rectal cancer
squamous cell carcinoma
pseudomonas aeruginosa
single cell
radiation therapy
mass spectrometry