A collagen-binding EGFR antibody fragment targeting tumors with a collagen-rich extracellular matrix

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作者
Hui Liang
Xiaoran Li
Bin Wang
Bing Chen
Yannan Zhao
Jie Sun
Yan Zhuang
Jiajia Shi
He Shen
Zhijun Zhang
Jianwu Dai
机构
[1] Key Laboratory for Nano-Bio Interface Research,Division of Nanobiomedicine
[2] Suzhou Institute of Nano-Tech and Nano-Bionics,undefined
[3] Chinese Academy of Sciences,undefined
[4] State Key Laboratory of Molecular Developmental Biology,undefined
[5] Institute of Genetics and Developmental Biology,undefined
[6] Chinese Academy of Sciences,undefined
[7] University of Chinese Academy of Sciences,undefined
来源
Scientific Reports | / 6卷
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摘要
Many tumors over-express collagen, which constitutes the physical scaffold of tumor microenvironment. Collagen has been considered to be a target for cancer therapy. The collagen-binding domain (CBD) is a short peptide, which could bind to collagen and achieve the sustained release of CBD-fused proteins in collagen scaffold. Here, a collagen-binding EGFR antibody fragment was designed and expressed for targeting the collagen-rich extracellular matrix in tumors. The antibody fragment (Fab) of cetuximab was fused with CBD (CBD-Fab) and expressed in Pichia pastoris. CBD-Fab maintained antigen binding and anti-tumor activity of cetuximab and obtained a collagen-binding ability in vitro. The results also showed CBD-Fab was mainly enriched in tumors and had longer retention time in tumors in A431 s.c. xenografts. Furthermore, CBD-Fab showed a similar therapeutic efficacy as cetuximab in A431 xenografts. Although CBD-Fab hasn’t showed better therapeutic effects than cetuximab, its smaller molecular and special target may be applicable as antibody–drug conjugates (ADC) or immunotoxins.
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