An epidermal growth factor receptor‐targeting immunotoxin based on IgG shows potent antitumor activity against head and neck cancer

Author:

Huang Mei1ORCID,Park Jisoo2ORCID,Seo Jina2ORCID,Ko Sanghwan3ORCID,Yang Yoon Hee4ORCID,Lee Yeaji2ORCID,Kim Hyo Jeong5ORCID,Lee Bok‐Soon5ORCID,Lee Yun Sang5ORCID,Ko Byoung Joon6ORCID,Jung Sang Teak378ORCID,Park Deachan29ORCID,Yoo Tae Hyeon29ORCID,Kim Chul‐Ho245ORCID

Affiliation:

1. Department of Medical Sciences Graduate School of Ajou University Suwon Republic of Korea

2. Department of Molecular Science and Technology Ajou University Suwon Republic of Korea

3. Department of Biomedical Sciences, Graduate School Korea University Seoul Republic of Korea

4. Department of Biomedical Sciences Graduate School of Ajou University Suwon Republic of Korea

5. Department of Otolaryngology Ajou University School of Medicine Suwon Republic of Korea

6. School of Biopharmaceutical and Medical Sciences Sungshin Women's University Seoul Republic of Korea

7. Institute of Human Genetics Korea University College of Medicine Seoul Republic of Korea

8. BK21 Graduate Program, Department of Biomedical Sciences Korea University College of Medicine Seoul Republic of Korea

9. Advanced College of Bio‐convergence Engineering Ajou University Suwon Republic of Korea

Abstract

AbstractThe epidermal growth factor receptor (EGFR) is an important target for cancer therapies. Many head and neck cancer (HNC) cells have been reported to overexpress EGFR; therefore, anti‐EGFR therapies have been attempted in patients with HNC. However, its clinical efficacy is limited owing to the development of drug resistance. In this study, we developed an EGFR‐targeting immunotoxin consisting of a clinically proven anti‐EGFR IgG (cetuximab; CTX) and a toxin fragment (LR‐LO10) derived from Pseudomonas exotoxin A (PE) using a novel site‐specific conjugation technology (peptide‐directed photo‐crosslinking reaction), as an alternative option. The immunotoxin (CTX‐LR‐LO10) showed specific binding to EGFR and properties of a typical IgG, such as stability, interactions with receptors of immune cells, and pharmacokinetics, and inhibited protein synthesis via modification of elongation factor‐2. Treatment of EGFR‐positive HNC cells with the immunotoxin resulted in apoptotic cell death and the inhibition of cell migration and invasion. The efficacy of CTX‐LR‐LO10 was evaluated in xenograft mouse models, and the immunotoxin exhibited much stronger tumor suppression than CTX or LR‐LO10. Transcriptome analyses revealed that the immunotoxins elicited immune responses and altered the expression of genes related to its mechanisms of action. These results support the notion that CTX‐LR‐LO10 may serve as a new therapeutic agent targeting EGFR‐positive cancers.

Funder

Korea Health Industry Development Institute

National Research Foundation of Korea

Publisher

Wiley

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