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

Author:

Qiu Weiyi1ORCID,Zhang Chang12,Wang Shuang1,Yu Xiaoyan1,Wang Qiong1,Zeng Dadi1,Du Peng1,Ma Jinling3,Zheng Yiqiong4,Pang Bo5,Yu Yunzhou1,Long Feng1,Pang Xiaobin2ORCID,Sun Zhiwei1ORCID

Affiliation:

1. Antibody Engineering Group, Beijing Biotechnology Institute, 100071 Beijing, China

2. Pharmaceutical Institute, Henan University, 475004 Kaifeng, China

3. Joinn Laboratories (China), Co. Ltd, 100176 Beijing, China

4. 301 Hospital, 100853 Beijing, China

5. Clinical Laboratory, Guang’anmen Hospital, China Academy of Chinese Medical Sciences, 100053 Beijing, China

Abstract

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.

Funder

National Science and Technology Major Project

Publisher

Hindawi Limited

Subject

Immunology,General Medicine,Immunology and Allergy

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