Abstract
"Tumor-Associated macrophages" (TAMs) form a significant cell population in malignant tumors and contribute to tumor growth, metastasis, and neovascularization. Gliomas are characterized by extensive neo-Angiogenesis, and knowledge of the role of TAMs in neovascularization is important for future anti-Angiogenic therapies. The phenotypes and functions of TAMs are heterogeneous and more
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