Development of a humanized anti-FABP4 monoclonal antibody for potential treatment of breast cancer

Jiaqing Hao; Rong Jin; Yanmei Yi; Xingshan Jiang; Jianyu Yu; Zhen Xu; Nicholas J. Schnicker; Michael S. Chimenti; Sonia L. Sugg; Bing Li

doi:10.1186/s13058-024-01873-y

Breast Cancer Research (Jul 2024)

Development of a humanized anti-FABP4 monoclonal antibody for potential treatment of breast cancer

Jiaqing Hao,
Rong Jin,
Yanmei Yi,
Xingshan Jiang,
Jianyu Yu,
Zhen Xu,
Nicholas J. Schnicker,
Michael S. Chimenti,
Sonia L. Sugg,
Bing Li

Affiliations

Jiaqing Hao: Department of Pathology, University of Iowa
Rong Jin: Department of Immunology, School of Basic Medical Sciences, Peking University
Yanmei Yi: School of Basic Medical Sciences, Guangdong Medical University
Xingshan Jiang: Department of Pathology, University of Iowa
Jianyu Yu: Department of Pathology, University of Iowa
Zhen Xu: Protein and Crystallography Facility, University of Iowa
Nicholas J. Schnicker: Protein and Crystallography Facility, University of Iowa
Michael S. Chimenti: Iowa Institute of Human Genetics, University of Iowa
Sonia L. Sugg: Department of Surgery, University of Iowa
Bing Li: Department of Pathology, University of Iowa

DOI: https://doi.org/10.1186/s13058-024-01873-y
Journal volume & issue: Vol. 26, no. 1
pp. 1 – 15

Abstract

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Abstract Background Breast cancer is the most common cancer in women diagnosed in the U.S. and worldwide. Obesity increases breast cancer risk without clear underlying molecular mechanisms. Our studies demonstrate that circulating adipose fatty acid binding protein (A-FABP, or FABP4) links obesity-induced dysregulated lipid metabolism and breast cancer risk, thus potentially offering a new target for breast cancer treatment. Methods We immunized FABP4 knockout mice with recombinant human FABP4 and screened hybridoma clones with specific binding to FABP4. The potential effects of antibodies on breast cancer cells in vitro were evaluated using migration, invasion, and limiting dilution assays. Tumor progression in vivo was evaluated in various types of tumorigenesis models including C57BL/6 mice, Balb/c mice, and SCID mice. The phenotype and function of immune cells in tumor microenvironment were characterized with multi-color flow cytometry. Tumor stemness was detected by ALDH assays. To characterize antigen-antibody binding capacity, we determined the dissociation constant of selected anti-FABP4 antibodies via surface plasmon resonance. Further analyses in tumor tissue were performed using 10X Genomics Visium spatial single cell technology. Results Herein, we report the generation of humanized monoclonal antibodies blocking FABP4 activity for breast cancer treatment in mouse models. One clone, named 12G2, which significantly reduced circulating levels of FABP4 and inhibited mammary tumor growth, was selected for further characterization. After confirming the therapeutic efficacy of the chimeric 12G2 monoclonal antibody consisting of mouse variable regions and human IgG1 constant regions, 16 humanized 12G2 monoclonal antibody variants were generated by grafting its complementary determining regions to selected human germline sequences. Humanized V9 monoclonal antibody showed consistent results in inhibiting mammary tumor growth and metastasis by affecting tumor cell mitochondrial metabolism. Conclusions Our current evidence suggests that targeting FABP4 with humanized monoclonal antibodies may represent a novel strategy for the treatment of breast cancer and possibly other obesity- associated diseases.

Published in Breast Cancer Research

ISSN: 1465-5411 (Print); 1465-542X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://breast-cancer-research.biomedcentral.com/

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