Matrix Stiffness Triggers Lipid Metabolic Cross-talk between Tumor and Stromal Cells to Mediate Bevacizumab Resistance in Colorectal Cancer Liver Metastases

Yannan Zheng; Rui Zhou; Jianan Cai; Nanyan Yang; Zhaowei Wen; Zhihua Zhang; Huiying Sun; Genjie Huang; Yijin Guan; Na Huang; Min Shi; Yulin Liao; Jianping Bin; Wangjun Liao

doi:10.1158/0008-5472.CAN-23-0025

Matrix Stiffness Triggers Lipid Metabolic Cross-talk between Tumor and Stromal Cells to Mediate Bevacizumab Resistance in Colorectal Cancer Liver Metastases

Cancer Res. 2023 Nov 1;83(21):3577-3592. doi: 10.1158/0008-5472.CAN-23-0025.

Authors

Yannan Zheng^#¹, Rui Zhou^#¹, Jianan Cai^#¹, Nanyan Yang¹, Zhaowei Wen¹, Zhihua Zhang¹, Huiying Sun¹, Genjie Huang¹, Yijin Guan¹, Na Huang¹, Min Shi¹, Yulin Liao², Jianping Bin², Wangjun Liao¹

Affiliations

¹ Department of Oncology, Nanfang Hospital, Southern Medical University, Guangzhou, Guangdong, China.
² Department of Cardiology, Nanfang Hospital, Southern Medical University, Guangzhou, Guangdong, China.

^# Contributed equally.

Abstract

Bevacizumab is an anti-VEGF monoclonal antibody that plays an important role in the combination treatment of advanced colorectal cancer. However, resistance remains a major hurdle limiting bevacizumab efficacy, highlighting the importance of identifying a mechanism of antiangiogenic therapy resistance. Here, we investigated biophysical properties of the extracellular matrix (ECM) related to metabolic processes and acquired resistance to bevacizumab. Evaluation of paired pre- and posttreatment samples of liver metastases from 20 colorectal cancer patients treated with combination bevacizumab therapy, including 10 responders and 10 nonresponders, indicated that ECM deposition in liver metastases and a highly activated fatty acid oxidation (FAO) pathway were elevated in nonresponders after antiangiogenic therapy compared with responders. In mouse models of liver metastatic colorectal cancer (mCRC), anti-VEGF increased ECM deposition and FAO in colorectal cancer cells, and treatment with the FAO inhibitor etomoxir enhanced the efficacy of antiangiogenic therapy. Hepatic stellate cells (HSC) were essential for matrix stiffness-mediated FAO in colon cancer cells. Matrix stiffness activated lipolysis in HSCs via the focal adhesion kinase (FAK)/yes-associated protein (YAP) pathway, and free fatty acids secreted by HSCs were absorbed as metabolic substrates and activated FAO in colon cancer cells. Suppressing HSC lipolysis using FAK and YAP inhibition enhanced the efficacy of anti-VEGF therapy. Together, these results indicate that bevacizumab-induced ECM remodeling triggers lipid metabolic cross-talk between colon cancer cells and HSCs. This metabolic mechanism of bevacizumab resistance mediated by the physical tumor microenvironment represents a potential therapeutic target for reversing drug resistance.

Significance: Extracellular matrix stiffening drives bevacizumab resistance by stimulating hepatic stellate cells to provide fuel for mCRC cells in the liver, indicating a potential metabolism-based therapeutic strategy for overcoming resistance.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Bevacizumab / pharmacology
Bevacizumab / therapeutic use
Colonic Neoplasms* / drug therapy
Colorectal Neoplasms* / pathology
Humans
Lipids
Liver Neoplasms* / pathology
Mice
Stromal Cells / metabolism
Tumor Microenvironment

Substances

Bevacizumab
Lipids