Abstract

The recruitment of hematopoietic bone marrow-derived cells by tumors has been previously reported. It has been shown that these precursors can secrete factors that modulate tissue vascularization, or can incorporate directly into the neovasculature acquiring endothelial or periciytic phenotypes. Moreover, once they have homed to the tumor, multipotent bone marrow precursors might also have the potential to become tumor- associated hematopoietic and mesenchymal cells. We have previously reported that under the influence of VEGF and 2-defensin, bone marrow-derived leukocytes expressing dendritic cell markers, are capable of contributing to tumor vasculature in a mouse model of ovarian cancer. A similar population was identified in human ovarian tumors. We called these cells vascular leukocytes (VLCs) since they expressed both hematopoietic and endothelial cell markers, and participate in neoangiogenesis. The co-expression of leukocyte and vascular markers suggests that these cells are part of the early steps of angiogenesis. Thus, we speculated that VLCs may originate from a hematopoietic precursor that could be attracted to the tumor microenvironment where it differentiates. In order to address this issue, we investigated changes in bone marrow populations induced by the development of distant tumors. We have performed preliminary experiments showing that in different mouse tumor models, a dramatic decrease in the proportion of hematopoietic bone marrow precursors is observed as tumor develops. In particular, we have observed relevant changes in the levels of a common precursor for B cells and dendritic cells (PBD). This stem cell population characterized by the coexpression of surface markers CD45, B220 and C1qRp (Early B lineage antigen/AA4.1), can generate B cells or dendritic cells in vitro depending on the cytokine milieu. Moreover, we have also detected PBDs in the microenvironment of mouse and human tumors. In the tumor, these cells express endothelial markers and proangiogenic molecules. Our general hypothesis is that bone marrow PBDs are attracted to the tumor microenvironment by specific chemokines, and there they differentiate into tumor-associated leukocytes with angiogenic capabilities. Involving undergraduate, graduate and medical students, this R15 proposal will critically examine several important mechanisms of the tumor-bone marrow interaction through the following specific aims:
Aim 1. Define the molecular profile of PBD cells recovered from bone marrow of naove animals or from the tumor microenvironment;
Aim 2. Determine the mechanisms involved in PBDs'capability to generate tumor- associated leukocyte populations (i.e., VLCs);
and Aim 3. Determine the mechanisms responsible for PBD migration towards the tumor microenvironment. Ultimately, these data will allow for a better understanding of the mechanisms by which bone marrow precursors participate in tumor development.

Public Health Relevance

Tumor vasculature represents a powerful new target of anti-cancer therapy. Novel targets of anti- angiogenic therapy include molecules which are uniquely expressed on tumor endothelium and/or endothelial precursors. In this project we will define the angiogenic properties of a new bone marrow precursor that can be attracted to the tumor microenvironment and contribute to neoangiogenesis. We believe this precursor represents potential targets for anti-vascular therapeutics.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Academic Research Enhancement Awards (AREA) (R15)
Project #
1R15CA137499-01
Application #
7575423
Study Section
Special Emphasis Panel (ZRG1-ONC-W (91))
Program Officer
Duglas-Tabor, Yvonne
Project Start
2009-01-01
Project End
2011-12-31
Budget Start
2009-01-01
Budget End
2011-12-31
Support Year
1
Fiscal Year
2009
Total Cost
$221,250
Indirect Cost

  Institution

Name
Ohio University Athens
Department
Other Basic Sciences
Type
Schools of Osteopathic Medicine
DUNS #
041077983
City
Athens
State
OH
Country
United States
Zip Code
45701

  Publications

Block, Keith I; Gyllenhaal, Charlotte; Lowe, Leroy et al. (2015) Designing a broad-spectrum integrative approach for cancer prevention and treatment. Semin Cancer Biol 35 Suppl:S276-S304
Casey, Stephanie C; Amedei, Amedeo; Aquilano, Katia et al. (2015) Cancer prevention and therapy through the modulation of the tumor microenvironment. Semin Cancer Biol 35 Suppl:S199-S223
Sprague, Leslee; Muccioli, Maria; Pate, Michelle et al. (2014) Dendritic cells: In vitro culture in two- and three-dimensional collagen systems and expression of collagen receptors in tumors and atherosclerotic microenvironments. Exp Cell Res 323:7-27
Caballero-Campo, Pedro; Buffone, Mariano G; Benencia, Fabian et al. (2014) A role for the chemokine receptor CCR6 in mammalian sperm motility and chemotaxis. J Cell Physiol 229:68-78
Benencia, Fabian (2014) Antigen-specific mRNA transfection of autologous dendritic cells. Methods Mol Biol 1139:77-86
Osterbur, Jacob; Sprague, Leslee; Muccioli, Maria et al. (2013) Adhesion to substrates induces dendritic cell endothelization and decreases immunological response. Immunobiology 218:64-75
Muccioli, Maria; Longstaff, Caitlin; Benencia, Fabian (2012) Absence of CD4 T-cell help provides a robust CD8 T-cell response while inducing effective memory in a preclinical model of melanoma. Immunotherapy 4:477-81
Muccioli, Maria; Pate, Michelle; Omosebi, Omowaleola et al. (2011) Generation and labeling of murine bone marrow-derived dendritic cells with Qdot nanocrystals for tracking studies. J Vis Exp :
Sprague, Leslee; Muccioli, Maria; Pate, Michelle et al. (2011) The interplay between surfaces and soluble factors define the immunologic and angiogenic properties of myeloid dendritic cells. BMC Immunol 12:35