| Literature DB >> 15488763 |
Li Yang1, Laura M DeBusk, Koari Fukuda, Barbara Fingleton, Brenda Green-Jarvis, Yu Shyr, Lynn M Matrisian, David P Carbone, P Charles Lin.
Abstract
We demonstrate a novel tumor-promoting role of myeloid immune suppressor Gr+CD11b+ cells, which are evident in cancer patients and tumor-bearing animals. These cells constitute approximately 5% of total cells in tumors. Tumors coinjected with Gr+CD11b+ cells exhibited increased vascular density, vascular maturation, and decreased necrosis. These immune cells produce high levels of MMP9. Deletion of MMP9 in these cells completely abolishes their tumor-promoting ability. Gr+CD11b+ cells were also found to directly incorporate into tumor endothelium. Consistent with this observation, Gr+CD11b+ cells acquire endothelial cell (EC) properties in tumor microenvironment and proangiogenic culture conditions. Our data provide evidence that Gr+CD11b+ cells of immune origin induced by tumors directly contribute to tumor growth and vascularization by producing MMP9 and differentiating into ECs.Entities:
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Year: 2004 PMID: 15488763 DOI: 10.1016/j.ccr.2004.08.031
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743