Abstract

Pancreatic cancers are particularly lethal and known for aggressive metastatic invasion. Over the prior funding period we have gathered substantial published and unpublished observations providing insight into how cells from these tumors disseminate. These findings support our CENTRAL HYPOTHESIS predicting that invasive pancreatic tumor cells and associated stromal cells in situ form a dynamic actin-based invadosome at the leading edge that selectively recruits specific metalloproteases to support adhesion, migration, and matrix remodeling during metastatic invasion. This hypothesis will test the contributions of the large polymeric GTPase Dynamin2 that forms a contractile scaffold linking the invadosome actin-based network to the advancing cell membrane. We will pursue three related but distinct specific aims that will provide mechanistic insights into the machinery, signaling, and degradative process utilized by invading PDAC cells and associated stroma.
These aims i nclude: One, defining the Dyn2/actin-based machinery that is essential for invadosome extension during migration in a 3-dimensional environment and in situ, with special emphasis on the expression, interaction, and function of the oncogenic actin adaptors, a-actinin 1 and 4, Two, understanding the regulation of invadosome dynamics by small oncogenic GTPases, that directly bind Dyn2, with an emphasis on a therapeutic approach, and Three, defining the mechanisms of matrix remodeling by the Dyn2- centric invadosome through the identification of novel pathways that regulate protease activity. This proposal will apply stat-of-the-art live-cell imaging methods to multiple experimental model systems that manipulate mixed populations of tumor and stromal cells in a 3D environment, as well as tumors resected from genetic mouse models and from human PDAC patients. The information gleaned from these approaches will greatly expand our mechanistic understanding of this disease while developing new therapies and treatments.

Public Health Relevance

Pancreatic cancers are particularly lethal and known for aggressive metastatic invasion. This proposal will provide new insights, concepts, and approaches toward defining the central mechanisms by which these tumor cells, and the associated stromal cells, migrate away from the pancreas to invade peripheral organs. State of the art live cell imaging methods will be applied to multiple experimental model systems that combine tumor with stromal cells in a native 3D environment, as well as tumors resected from genetic mouse models and from human PDAC patients. The information gleaned from these approaches will greatly expand our mechanistic understanding of this disease for application toward new therapies and treatments

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA104125-15
Application #
9774747
Study Section
Clinical, Integrative and Molecular Gastroenterology Study Section (CIMG)
Program Officer
Ault, Grace S
Project Start
2003-12-01
Project End
2020-07-31
Budget Start
2019-08-01
Budget End
2020-07-31
Support Year
15
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Razidlo, Gina L; Burton, Kevin M; McNiven, Mark A (2018) Interleukin-6 promotes pancreatic cancer cell migration by rapidly activating the small GTPase CDC42. J Biol Chem 293:11143-11153
Zhu, Shizhen; Zhang, Xiaoling; Weichert-Leahey, Nina et al. (2017) LMO1 Synergizes with MYCN to Promote Neuroblastoma Initiation and Metastasis. Cancer Cell 32:310-323.e5
Boddicker, Rebecca L; Razidlo, Gina L; Feldman, Andrew L (2016) Genetic alterations affecting GTPases and T-cell receptor signaling in peripheral T-cell lymphomas. Small GTPases :1-7
Boddicker, Rebecca L; Razidlo, Gina L; Dasari, Surendra et al. (2016) Integrated mate-pair and RNA sequencing identifies novel, targetable gene fusions in peripheral T-cell lymphoma. Blood 128:1234-45
Cao, Hong; Eppinga, Robbin D; Razidlo, Gina L et al. (2016) Stromal fibroblasts facilitate cancer cell invasion by a novel invadopodia-independent matrix degradation process. Oncogene 35:1099-1110
Razidlo, Gina L; Magnine, Christopher; Sletten, Arthur C et al. (2015) Targeting Pancreatic Cancer Metastasis by Inhibition of Vav1, a Driver of Tumor Cell Invasion. Cancer Res 75:2907-15
Razidlo, Gina L; Schroeder, Barbara; Chen, Jing et al. (2014) Vav1 as a central regulator of invadopodia assembly. Curr Biol 24:86-93
McNiven, Mark A (2013) Breaking away: matrix remodeling from the leading edge. Trends Cell Biol 23:16-21
Razidlo, Gina L; Wang, Yu; Chen, Jing et al. (2013) Dynamin 2 potentiates invasive migration of pancreatic tumor cells through stabilization of the Rac1 GEF Vav1. Dev Cell 24:573-85
Feng, H; Liu, K W; Guo, P et al. (2012) Dynamin 2 mediates PDGFR?-SHP-2-promoted glioblastoma growth and invasion. Oncogene 31:2691-702

Showing the most recent 10 out of 22 publications