Angiogenesis
normoxic conditions
VHL degrades HIF during normoxia, makes for degradation
VEGF
cells monitor O2 tension through VHL proteins under hypoxic conditions VHL proteins signal for production and release of VEGF VEGF binds to receptors on the surface of endothelial cells stimulating their proliferation endothelial cells also migrate towards areas of higher VEGF concentration angiogenic factor
heterotypic interactions
heterogenous cell communication
what promotes angiogenesis?
hypoxia oncogenes
vasculature increases pressure
leakiness of tumor vasculature results in increased interstitial pressure lower pressure in tumor veins higher interstitial pressure lowers effective penetration of drugs
angiogenic switch
normal conditions prevent cells from triggering angiogenesis as tumors progress they gain the capacity to promote angiogenesis thus, overcoming the normal inhibition of angiogenesis
how are new vessels formed?
pre-existing vessels endothelial progenitor cells from the bone marrow
why do tumors induce angiogenesis?
provides nutrients required for cell growth provides a roadway for metastatic spread promotes tumor growth and spread
thrombospondin-1
secreted by many cell types is boudn to molecules in the ECM binds to receptors (cd36/47) on the surface of endothelial cells inhibits endothelial cell proliferation
stromal cells
streams cell release many cytokines and growth factors also produce MMPs and other proteases heterotypic interactions with storm enhance angiogenesis
VHL mutations
these mutations result in constitutively active HIF VHL and VEGF expression are inversely related
how far can tumors be from a blood vessel?
0.2 mm
angiogenesis pathway
1. hypoxic response elements cause tumor cells to up regulate pro-angiogenic factors 2. pro-angiogenic factors activate endothelial cells to increase proliferation 3. MMP are activated by tumor cells and endothelial cells to permit further endothelial cell growth and migration 4. Tumor vascularity is increased
tumor capillaries
3 times the diameter disorganized loosely associated parasites gaps between cells walls are more permeable higher interstitial fluid pressure poor lymphatic drainage
hypoxic conditions
HIF activates VEGF during hypoxia
when does angiogenesis happen?
embryonic development growth implantation of placenta uterine lining wound healing non-malignant disease: diabetic retinopathy, psoriasis, RA malignant disease: tumorogenesis
angiogenesis defined
growth of new blood vessels from preexisting blood vessels
can attract calls from distant sites (heterotypic interactions)
tumor cells may attract local endothelial cells, but can also attract precursor cells from distant sites like the bone marrow releases ECM bound angiogenic factors promotes endothelial cell migration through ECM allows for direct access of tumor to new vessels vasodilators are expressed chemokine and growth factors are also expressed
streams cells (heterotypic interactions)
tumor cells may attract other stream cell types that promote angiogenesis
degradation of the ECM and basement membrane (heterotypic interactions)
tumor cells may release enzymes, MMP, that degrade ECM and basement membrane releases ECM bound angiogenic factors promotes endothelial cell migration through ECM allows for direct access of tumor to new vessels
creating new vessels
tumors don't take over existing vessels they secrete angiogenic factors to stimulate the growth of new vessels from normal cells
