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Characterization of tumors produced by signal peptide-basic fibroblast growth factor-transformed cells.

作者信息

Rogelj S, Weinberg R A, Fanning P, Klagsbrun M

机构信息

Whitehead Institute for Biomedical Research, Cambridge, Massachusetts 02142.

出版信息

J Cell Biochem. 1989 Jan;39(1):13-23. doi: 10.1002/jcb.240390103.

DOI:10.1002/jcb.240390103
PMID:2469690
Abstract

Basic fibroblast growth factor (bFGF) is found in a variety of cells and tissues. We have previously shown that bFGF is a transforming growth factor, but only when fused to a signal peptide (sp-bFGF). Cells expressing the native bFGF are tumorigenic in nude mice only, where the tumors form at a low frequency and grow very slowly as compared to sp-bFGF tumors. The cells transformed by the sp-bFGF growth factor gene cause rapidly growing tumors within 10 days in 100% of syngeneic and nude mice. In nude mice, the tumors are highly vascularized, while the vascularization in immunocompetent syngeneic mice is not as prominent. The syngeneic mice have a characteristic humoral immune response to sp-bFGF tumors, which differs from that mounted against ras-induced tumors. The ability of bFGF to induce tumorigenicity is significant in view of the recent discoveries of three new oncogenes: hst, int-2, and an oncogene from a human colon cancer. In addition to homology with FGF, the proteins encoded by these oncogenes all have a potential signal peptide at the protein's amino terminus, suggesting a mode of action analogous to that of our artificial signal peptide-bFGF (sp-bFGF) transforming growth factor model system.

摘要

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