Anti-tumor effects of fibroblast growth factor-binding protein (FGF-BP) knockdown in colon carcinoma

D Schulze, P Plohmann, S Höbel, A Aigner - Molecular Cancer, 2011 - Springer
D Schulze, P Plohmann, S Höbel, A Aigner
Molecular Cancer, 2011Springer
Background Fibroblast growth factors FGF-1 and FGF-2 are often upregulated in tumors, but
tightly bound to heparan sulphate proteoglycans of the extracellular matrix (ECM). One
mechanism of their bioactivation relies on the FGF-binding protein (FGF-BP) which, upon
reversible binding to FGF-1 or-2, leads to their release from the ECM. FGF-BP increases
tumorigenicity and is highly expressed in tumors like colon carcinoma. In this paper, we
analyse cellular and molecular consequences of RNAi-mediated FGF-BP knockdown in …
Background
Fibroblast growth factors FGF-1 and FGF-2 are often upregulated in tumors, but tightly bound to heparan sulphate proteoglycans of the extracellular matrix (ECM). One mechanism of their bioactivation relies on the FGF-binding protein (FGF-BP) which, upon reversible binding to FGF-1 or -2, leads to their release from the ECM. FGF-BP increases tumorigenicity and is highly expressed in tumors like colon carcinoma. In this paper, we analyse cellular and molecular consequences of RNAi-mediated FGF-BP knockdown in colon carcinoma, and explore the therapeutic effects of the nanoparticle-mediated delivery of small interfering RNAs (siRNAs) for FGF-BP targeting.
Results
Employing stable RNAi cells, we establish a dose-dependence of cell proliferation on FGF-BP expression levels. Decreased proliferation is mirrored by alterations in cell cycle distribution and upregulation of p21, which is relevant for mediating FGF-BP effects. While inhibition of proliferation is mainly associated with reduced Akt and increased GSK3β activation, antibody array-based analyses also reveal other alterations in MAPK signalling. Additionally, we demonstrate induction of apoptosis, mediated through caspase-3/7 activation, and alterations in redox status upon FGF-BP knockdown. These effects are based on the upregulation of Bad, Bax and HIF-1α, and the downregulation of catalase. In a therapeutic FGF-BP knockdown approach based on RNAi, we employ polymer-based nanoparticles for the in vivo delivery of siRNAs into established wildtype colon carcinoma xenografts. We show that the systemic treatment of mice leads to the inhibition of tumor growth based on FGF-BP knockdown.
Conclusions
FGF-BP is integrated in a complex network of cytoprotective effects, and represents a promising therapeutic target for RNAi-based knockdown approaches.
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