| Literature DB >> 12429975 |
Yasushi Tomii1, Hitoshi Yamazaki, Nobuko Sawa, Yasuyuki Ohnishi, Junichiro Kamochi, Tetsuji Tokunaga, Yoshiyuki Osamura, Sotaro Sadahiro, Hiroshi Kijima, Yoshiyuki Abe, Yoshito Ueyama, Norikazu Tamaoki, Masato Nakamura.
Abstract
The 189 amino acid isoform of vascular endothelial growth factor (VEGF189) has been shown to be more strongly associated with the cell membrane than other isoforms of human VEGF (VEGF121, VEGF165). To analyze the biological activities of these VEGF isoforms on tumor growth, we transfected human VEGF121, VEGF165 or VEGF189 cDNA into the human colon cancer cell line SW-480, and established several clones overexpressing these VEGF isoforms. The total amounts of VEGF protein in the culture supernatants of the VEGF189-transfectants were less than those of VEGF121 and VEGF165-transfectants. These transfectants showed no significant differences in growth in culture. Nevertheless, the rate of in vivo tumor growth of VEGF189-transfectants was faster than or equivalent to that of VEGF121-transfectants, while the VEGF165-transfectant showed the greatest enhancement of tumor growth. The protein levels of VEGF were markedly increased only in the VEGF189-transfectants cultured in the presence of heparin. The enhanced in vivo tumor growth of VEGF189-transfectants can be partly explained by the cell-associated features of VEGF189 molecules. The VEGF189 molecule, which is strongly bound to the cell surface, has unique properties and high potential in local angiogenesis and tumor growth in the cancer inductive microenvironment.Entities:
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Year: 2002 PMID: 12429975
Source DB: PubMed Journal: Int J Oncol ISSN: 1019-6439 Impact factor: 5.650