Title of article :
Myeloid cell trafficking and tumor angiogenesis
Author/Authors :
Schmid، نويسنده , , Michael C. and Varner، نويسنده , , Judith A.، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 2007
Abstract :
Tumor growth and metastasis depend on neovascularization, the growth of new blood vessels. Recent findings have revealed that tumor neovascularization is regulated in part by monocytes, which are myeloid lineage cells from the bone marrow. Tumors exhibit significant monocyte infiltrates, which are actively recruited to the tumor microenvironment. Upon tumor infiltration, monocytes can participate in tumor neovascularization. Monocytes can either differentiate into macrophages, which express proangiogenic growth factors, or into endothelial-like cells, which may directly participate in neovascularization. Preliminary studies in animals suggest that modulation of bone marrow-derived cell trafficking into tumors will provide a useful new approach in cancer therapy.
Keywords :
Monocyte , Progenitor cell , Angiogenesis , Integrin , Chemokine , Endothelial progenitor cell
Journal title :
Cancer Letters
Journal title :
Cancer Letters