Whiles significant progress has been made in the development of new therapeutics to control malignant melanoma, the overall 5-year survival of patients with metastatic disease remains low in the majority of treated subjects. Thus, there is an urgent need for a more detailed understanding of how immune and inflammatory mechanisms govern melanoma progression in order to enhance long-term durable responses in a larger percentage of patients. Evidence indicates that immune infiltrates within the tumor microenvironment such as macrophages play critical roles in angiogenesis, tumor growth and escape from immune control. Melanomas often use an adaptive strategy of actively reprogramming stromal elements towards an immunosuppressive phenotype. Tumor associated macrophages (TAM) can modify both endothelial and T-cell behavior, thereby regulating angiogenesis, tumor growth and the efficacy of many cancer therapies. Identifying novel pro- angiogenic and immune suppressive factors generated by TAMs may provide new therapeutic opportunities and contribute to a more in depth understanding of how the tumor microenvironment controls melanoma growth. To this end, we made the surprising observation that an evolutionarily conserved RGDKGE containing collagen epitope can be generated by M2-like macrophages, and its expression was elevated over 3-fold within the circulation of a cohort of melanoma patients. Remarkably, this RGDKGE collagen epitope, but not other RGD collagen peptides, enhanced endothelial cell growth, stress fiber formation, nuclear translocation of the Yes-associated protein YAP, and induced a dose-dependent angiogenic and pro-inflammatory response in vivo. Based on these and other data, we will test the hypothesis that the RGDKGE epitope regulates angiogenesis and tumor growth by a novel integrin-YAP-dependent mechano-transduction pathway leading to the initiation of a pro-angiogenic signaling program.

Public Health Relevance

Identifying a previously unrecognized mechanism by which tumor-associated macrophages generate a pro- angiogenic and immunosuppressive collagen fragment that regulates melanoma growth may lead to the development of more effective treatment strategies. The proposal will test the hypothesis that a highly conserved RGDKGE containing collagen epitope regulates angiogenesis and tumor growth by a novel integrin- YAP-dependent mechano-transduction pathway leading to the initiation of a pro-angiogenic and inflammatory signaling program. Our studies will contribute to a more in-depth molecular understanding of the mechanisms by which cooperative interactions between distinct stromal cell compartments regulates angiogenesis and tumor growth and may contribute to the development of a new treatment paradigm for more effective and durable management for malignant melanoma.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA196739-04
Application #
9828644
Study Section
Tumor Progression and Metastasis Study Section (TPM)
Program Officer
Woodhouse, Elizabeth
Project Start
2016-12-05
Project End
2021-11-30
Budget Start
2019-12-01
Budget End
2020-11-30
Support Year
4
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Mainehealth
Department
Type
DUNS #
071732663
City
Portland
State
ME
Country
United States
Zip Code
04102
Caron, Jennifer M; Han, XiangHua; Contois, Liangru et al. (2018) The HU177 Collagen Epitope Controls Melanoma Cell Migration and Experimental Metastasis by a CDK5/YAP-Dependent Mechanism. Am J Pathol 188:2356-2368