Proteolytic processing regulates receptor specificity and activity of VEGF-C

Abstract: The recently identified vascular endothelial growth factor C (VEGF-C) belongs to the platelet-derived growth factor (PDGF)/VEGF family of growth factors and is a ligand for the endothelial-specific receptor tyrosine kinases VEGFR-3 and VEGFR-2. The VEGF homology domain spans only about one-third of the cysteine-rich VEGF-C precursor. Here we have analysed the role of post-translational processing in VEGF-C secretion and function, as well as the structure of the mature VEGF-C. The stepwise proteolytic processin… Show more

“…We found that VEGF-C downregulation was accompanied by reappearance of certain traits of epithelial phenotype and a decrease in expression of mesenchymal markers that was observed in both A549 ( Figure 6) and HCT116 cells (Supplementary Immature forms of VEGF-C bind only to VEGFR3; mature form binds to VEGFR3 with higher affinity than immature forms, and additionally interacts with VEGFR2 (Joukov et al, 1997). a-tubulin protein was analyzed as loading control.…”

Downregulation of VEGF-C expression in lung and colon cancer cells decelerates tumor growth and inhibits metastasis via multiple mechanisms

“…We found that VEGF-C downregulation was accompanied by reappearance of certain traits of epithelial phenotype and a decrease in expression of mesenchymal markers that was observed in both A549 ( Figure 6) and HCT116 cells (Supplementary Immature forms of VEGF-C bind only to VEGFR3; mature form binds to VEGFR3 with higher affinity than immature forms, and additionally interacts with VEGFR2 (Joukov et al, 1997). a-tubulin protein was analyzed as loading control.…”

Downregulation of VEGF-C expression in lung and colon cancer cells decelerates tumor growth and inhibits metastasis via multiple mechanisms

“…Subsequently, the propeptides can be proteolytically removed to generate mature forms consisting of VHD dimers. The full-length forms of both growth factors bind the lymphangiogenic receptor VEGFR-3 but the mature forms do so with greater affinity (Joukov et al, 1997;Stacker et al, 1999), suggesting that the degree of proteolytic processing of VEGF-C and VEGF-D may in part determine the extent of lymphangiogenesis induced by these proteins in a tumour. Once VEGF-C is processed to the mature form it acquires the capacity to bind VEGFR-2 (Joukov et al, 1997), a cell surface receptor tyrosine kinase thought to signal for angiogenesis.…”

“…The full-length forms of both growth factors bind the lymphangiogenic receptor VEGFR-3 but the mature forms do so with greater affinity (Joukov et al, 1997;Stacker et al, 1999), suggesting that the degree of proteolytic processing of VEGF-C and VEGF-D may in part determine the extent of lymphangiogenesis induced by these proteins in a tumour. Once VEGF-C is processed to the mature form it acquires the capacity to bind VEGFR-2 (Joukov et al, 1997), a cell surface receptor tyrosine kinase thought to signal for angiogenesis. In the case of VEGF-D, the affinity for VEGFR-2 is increased approximately 290-fold by proteolytic conversion of the full-length to the mature form (Stacker et al, 1999).…”

Targeting lymphangiogenesis to prevent tumour metastasis

“…In vitro studies have shown that VEGF-C and VEGF-D exhibit mitogenic effects for vascular and lymphatic endothelial cells and survival-promoting abilities for lymphatic endothelial cells through VEGFR3 Achen et al, 1998;Marconcini et al, 1999;Veikkola et al, 2001). Both growth factors promote angiogenesis in in vitro assays (Joukov et al, 1996;Joukov et al, 1997;Marconcini et al, 1999). Vascular endothelial growth factor-C promotes the formation of capillary-tube structures by lymphatic endothelial cells, but not blood vascular endothelial cells, in a collagen sandwich assay (Podgrabinska et al, 2002).…”

Vascular endothelial growth factors C and D and lymphangiogenesis in gastrointestinal tract malignancy