Abstract

Metastatic tumor cells are distinguished by their ability to invade the basement membrane of epithelial barriers and migrate to distant sites. Recent studies from this program demonstrate that host macrophages are critical for the motility and invasion of tumor cells, due to a paracrine loop involving the mutual signaling and chemotaxis between macrophages and tumor cells. PI3K is a critical regulator of cell motility, and distinct PI3K isoforms are required for regulation of actin-based motility in tumor cells versus macrophages. We propose to use isoform-specific inhibitors of Class IA PISKs as well as genetic approaches to examine the requirement for PI3K-mediated motility of both tumor cells and macrophages during invasion and metastasis. By selectively inhibiting the motility of tumor cells versus macrophages, we will test whether the enhanced tumor cell chemotaxis observed in the presence of macrophages requires pre-exposure to macrophage-derived cytokines, versus the presence of continuous macrophage signaling during coordinated migration of the two cell types. We will also examine the metastatic behavior of tumor cells expressing activating mutations of PI3K that are commonly found in human breast cancer. The unique assays developed by this program will allow a detailed analysis of how oncogenic p110ct mutants affect the tumor cell-macrophage paracrine loop. Finally, studies from this program have shown that genes coding for proteins that modulate the myosin-ll regulatory pathway are up-regulated in invasive tumor cells and that the amoeboid motility of tumor cells in a 3D matrix is mediated by the myosin-ll regulatory pathway. Given these findings, and our observations that PI3K regulates myosin-ll-based contractility in tumor cells, we will examine the PI3K isoform-dependence of myosin-ll phosphorylation, the identification of intermediary signaling pathways in tumor cells and macrophages, and the subsequent effects on motility and invasion. These studies will complete our analysis of the motility cycle as it relates to the invasion signature, and lead to new insights into the role of macrophage-tumor cell paracrine signaling during metastasis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA100324-08
Application #
8097229
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2010-06-01
Budget End
2011-05-31
Support Year
8
Fiscal Year
2010
Total Cost
$245,321
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Type
DUNS #
110521739
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Suyama, Kimita; Yao, Jiahong; Liang, Huizhi et al. (2018) An Akt3 Splice Variant Lacking the Serine 472 Phosphorylation Site Promotes Apoptosis and Suppresses Mammary Tumorigenesis. Cancer Res 78:103-114
Pastoriza, Jessica M; Karagiannis, George S; Lin, Juan et al. (2018) Black race and distant recurrence after neoadjuvant or adjuvant chemotherapy in breast cancer. Clin Exp Metastasis 35:613-623
Arwert, Esther N; Harney, Allison S; Entenberg, David et al. (2018) A Unidirectional Transition from Migratory to Perivascular Macrophage Is Required for Tumor Cell Intravasation. Cell Rep 23:1239-1248
Gizzi, Anthony S; Grove, Tyler L; Arnold, Jamie J et al. (2018) A naturally occurring antiviral ribonucleotide encoded by the human genome. Nature 558:610-614
Karagiannis, George S; Condeelis, John S; Oktay, Maja H (2018) Chemotherapy-induced metastasis: mechanisms and translational opportunities. Clin Exp Metastasis 35:269-284
Yang, Ming; McKay, Daniel; Pollard, Jeffrey W et al. (2018) Diverse Functions of Macrophages in Different Tumor Microenvironments. Cancer Res 78:5492-5503
Cabrera, Ramon M; Mao, Serena P H; Surve, Chinmay R et al. (2018) A novel neuregulin - jagged1 paracrine loop in breast cancer transendothelial migration. Breast Cancer Res 20:24
Meirson, Tomer; Genna, Alessandro; Lukic, Nikola et al. (2018) Targeting invadopodia-mediated breast cancer metastasis by using ABL kinase inhibitors. Oncotarget 9:22158-22183
Dulyaninova, Natalya G; Ruiz, Penelope D; Gamble, Matthew J et al. (2018) S100A4 regulates macrophage invasion by distinct myosin-dependent and myosin-independent mechanisms. Mol Biol Cell 29:632-642
Liu, Xia; Taftaf, Rokana; Kawaguchi, Madoka et al. (2018) Homophilic CD44 Interactions Mediate Tumor Cell Aggregation and Polyclonal Metastasis in Patient-Derived Breast Cancer Models. Cancer Discov :

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