Inhibition of tumor angiogenesis by oral etoposide
The chemotherapeutic agent etoposide is a topoisomerase II inhibitor widely used for cancer therapy. Low-dose oral etoposide, administered at close regular intervals, has potent anti-tumor activity in patients who are refractory to intravenous etoposide; however, the mechanism remains unclear. Since...
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| Veröffentlicht in: | Experimental and therapeutic medicine 2010-09, Vol.1 (5), p.739-746 |
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| creator | PANIGRAHY, DIPAK KAIPAINEN, ARJA BUTTERFIELD, CATHERINE E CHAPONIS, DEVINEY M LAFORME, ANDREA M FOLKMAN, JUDAH KIERAN, MARK W |
| description | The chemotherapeutic agent etoposide is a topoisomerase II inhibitor widely used for cancer therapy. Low-dose oral etoposide, administered at close regular intervals, has potent anti-tumor activity in patients who are refractory to intravenous etoposide; however, the mechanism remains unclear. Since endothelial cells may be more sensitive than tumor cells to chemotherapy agents, we determined the effects of etoposide alone and in combination with oral cyclooxygenase-2 inhibitors and peroxisome-proliferator activated receptor γ ligands on angiogenesis and tumor growth in xenograft tumor models. Optimal anti-angiogenic (metronomic) and anti-tumor doses of etoposide on angiogenesis, primary tumor growth and metastasis were established alone and in combination therapy. Etoposide inhibited endothelial and tumor cell proliferation, decreased vascular endothelial growth factor (VEGF) production by tumor cells and suppressed endothelial tube formation at non-cytotoxic concentrations. In our in vivo studies, oral etoposide inhibited fibroblast growth factor 2 and VEGF-induced corneal neovascularization, VEGF-induced vascular permeability and increased levels of the endogenous angiogenesis inhibitor endostatin in mice. In addition, etoposide inhibited Lewis lung carcinoma (LLC) and human glioblastoma (U87) primary tumor growth as well as spontaneous lung metastasis in a LLC resection model. Furthermore, etoposide had synergistic anti-tumor activity in combination with celecoxib and rosiglitazone, which are also oral anti-angiogenic and anti-tumor agents. Etoposide inhibits angiogenesis in vitro and in vivo by indirect and direct mechanisms of action. Combining etoposide with celecoxib and rosiglitazone increases its efficacy and merits further investigation in future clinical trials to determine the potential usefulness of etoposide in combinatory anti-angiogenic chemotherapy. |
| doi_str_mv | 10.3892/etm.2010.127 |
| format | Article |
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Low-dose oral etoposide, administered at close regular intervals, has potent anti-tumor activity in patients who are refractory to intravenous etoposide; however, the mechanism remains unclear. Since endothelial cells may be more sensitive than tumor cells to chemotherapy agents, we determined the effects of etoposide alone and in combination with oral cyclooxygenase-2 inhibitors and peroxisome-proliferator activated receptor γ ligands on angiogenesis and tumor growth in xenograft tumor models. Optimal anti-angiogenic (metronomic) and anti-tumor doses of etoposide on angiogenesis, primary tumor growth and metastasis were established alone and in combination therapy. Etoposide inhibited endothelial and tumor cell proliferation, decreased vascular endothelial growth factor (VEGF) production by tumor cells and suppressed endothelial tube formation at non-cytotoxic concentrations. In our in vivo studies, oral etoposide inhibited fibroblast growth factor 2 and VEGF-induced corneal neovascularization, VEGF-induced vascular permeability and increased levels of the endogenous angiogenesis inhibitor endostatin in mice. In addition, etoposide inhibited Lewis lung carcinoma (LLC) and human glioblastoma (U87) primary tumor growth as well as spontaneous lung metastasis in a LLC resection model. Furthermore, etoposide had synergistic anti-tumor activity in combination with celecoxib and rosiglitazone, which are also oral anti-angiogenic and anti-tumor agents. Etoposide inhibits angiogenesis in vitro and in vivo by indirect and direct mechanisms of action. 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Low-dose oral etoposide, administered at close regular intervals, has potent anti-tumor activity in patients who are refractory to intravenous etoposide; however, the mechanism remains unclear. Since endothelial cells may be more sensitive than tumor cells to chemotherapy agents, we determined the effects of etoposide alone and in combination with oral cyclooxygenase-2 inhibitors and peroxisome-proliferator activated receptor γ ligands on angiogenesis and tumor growth in xenograft tumor models. Optimal anti-angiogenic (metronomic) and anti-tumor doses of etoposide on angiogenesis, primary tumor growth and metastasis were established alone and in combination therapy. Etoposide inhibited endothelial and tumor cell proliferation, decreased vascular endothelial growth factor (VEGF) production by tumor cells and suppressed endothelial tube formation at non-cytotoxic concentrations. In our in vivo studies, oral etoposide inhibited fibroblast growth factor 2 and VEGF-induced corneal neovascularization, VEGF-induced vascular permeability and increased levels of the endogenous angiogenesis inhibitor endostatin in mice. In addition, etoposide inhibited Lewis lung carcinoma (LLC) and human glioblastoma (U87) primary tumor growth as well as spontaneous lung metastasis in a LLC resection model. Furthermore, etoposide had synergistic anti-tumor activity in combination with celecoxib and rosiglitazone, which are also oral anti-angiogenic and anti-tumor agents. Etoposide inhibits angiogenesis in vitro and in vivo by indirect and direct mechanisms of action. Combining etoposide with celecoxib and rosiglitazone increases its efficacy and merits further investigation in future clinical trials to determine the potential usefulness of etoposide in combinatory anti-angiogenic chemotherapy.</description><subject>etoposide</subject><subject>metronomic chemotherapy</subject><subject>oral combination therapy</subject><subject>peroxisome-proliferator activated receptor</subject><subject>tumor angiogenesis</subject><issn>1792-0981</issn><issn>1792-1015</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2010</creationdate><recordtype>article</recordtype><recordid>eNpVkM9LwzAUx4MoTuZunqU3PdiZpE2aXAQZ_hgMvOg5pEm6RdqkNqmw_96MzaG5vDzeh-97fAC4QnBeMI7vTezmGKYO4eoEXKCK4xxBRE4Pf8gZmoBZCJ8wPUIRY-QcTDDmvCC8ugB46Ta2ttF6l_kmi2Pnh0y6tfVr40ywIau3mR9km5noex-sNpfgrJFtMLNDnYKP56f3xWu-entZLh5XuSoRjXndSFlrRHnNSiWZIjB1vCS4INRQbTgziFGpVVlzSTRXmCFGeMOZRLIiqJiCh31uP9ad0cq4mO4Q_WA7OWyFl1b8nzi7EWv_LYqyJJzQFHB7CBj812hCFJ0NyrStdMaPQezW0YoRShJ6t0fV4EMYTHNcg6DYmRbJtNiZFsl0wq__nnaEf70m4GYPhF46bbUPRyYF5RDlkOSwKnjxA2qTh3A</recordid><startdate>20100901</startdate><enddate>20100901</enddate><creator>PANIGRAHY, DIPAK</creator><creator>KAIPAINEN, ARJA</creator><creator>BUTTERFIELD, CATHERINE E</creator><creator>CHAPONIS, DEVINEY M</creator><creator>LAFORME, ANDREA M</creator><creator>FOLKMAN, JUDAH</creator><creator>KIERAN, MARK W</creator><general>D.A. 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| subjects | etoposide metronomic chemotherapy oral combination therapy peroxisome-proliferator activated receptor tumor angiogenesis |
| title | Inhibition of tumor angiogenesis by oral etoposide |
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