Stat1 negatively regulates angiogenesis, tumorigenicity and metastasis of tumor cells

S Huang, CD Bucana, MV Arsdall, IJ Fidler - Oncogene, 2002 - nature.com
S Huang, CD Bucana, MV Arsdall, IJ Fidler
Oncogene, 2002nature.com
Stat1 is deficient or inactive in many types of human tumors whereas some tumors have
activated Stat1. Whether Stat1 affects tumor growth and metastasis is unclear. In the present
study, we used Stat1 knockout tumor cells to determine (1) whether Stat1 can regulate
angiogenesis, growth, and metastasis of tumor cells; and (2) whether Stat1 is required for
the inhibitory effect of IFN-β on the expression of angiogenic factor bFGF. Highly tumorigenic
and metastatic RAD-105 tumor cells derived from a fibrosarcoma of a Stat1 knockout mouse …
Abstract
Stat1 is deficient or inactive in many types of human tumors whereas some tumors have activated Stat1. Whether Stat1 affects tumor growth and metastasis is unclear. In the present study, we used Stat1 knockout tumor cells to determine (1) whether Stat1 can regulate angiogenesis, growth, and metastasis of tumor cells; and (2) whether Stat1 is required for the inhibitory effect of IFN-β on the expression of angiogenic factor bFGF. Highly tumorigenic and metastatic RAD-105 tumor cells derived from a fibrosarcoma of a Stat1 knockout mouse were reconstituted with a Stat1 expression vector. The reconstitution of Stat1 suppressed the tumorigenicity and metastasis of RAD-105 cells in nude mice which correlated with a decreased microvessel density and decreased expression of proangiogenic molecules bFGF, MMP-2, and MMP-9 in vivo. Moreover, noncytotoxic concentrations of IFN-β significantly inhibited the in vitro expression of bFGF in the Stat1-reconstituted cells but not in the Stat1-deficient cells, which was consistent with decreased bFGF expression of Stat1-reconstituted tumors in vivo. Therefore, Stat1 is essential for IFN-mediated inhibition of bFGF production, suggesting that tumor-intrinsic Stat1 is an important mediator for antiangiogenic signals, such as IFN. Collectively, these data demonstrate that Stat1 expressed by tumor cells is a negative regulator of tumor angiogenesis and, hence, tumor growth and metastasis.
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