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bFGF induces changes in hyaluronan synthase and hyaluronidase isoform expression and modulates the migration capacity of fibrosarcoma cells
Authors:Aikaterini Berdiaki  Dragana Nikitovic  Aristeidis Tsatsakis  Pavlos Katonis  Nikos K Karamanos  George N Tzanakakis
Institution:1. Department of Histology, Division of Morphology, School of Medicine, University of Crete, 71110, Heraklion, Greece;2. Department of Orthopedics, University Hospital of Heraklion, 71003, Heraklion, Greece;3. Laboratory of Biochemistry, Department of Chemistry, University of Patras, 26110, Patras, Greece
Abstract:

Background

Hyaluronan (HA) a glycosaminoglycan, is capable of transmitting extracellular matrix derived signals to regulate cellular functions. In this study, we investigated whether the changes in HT1080 and B6FS fibrosarcoma cell lines HA metabolism induced by basic fibroblast growth factor (bFGF) are correlated to their migration.

Methods

Real-time PCR, in vitro wound healing assay, siRNA transfection, enzyme digestions, western blotting and immunofluorescence were utilized.

Results

bFGF inhibited the degradation of HA by decreasing hyaluronidase-2 expression in HT1080 cells (p = 0.0028), increased HA-synthase-1 and -2 expression as we previously found and enhanced high molecular weight HA deposition in the pericellular matrix. Increased endogenous HA production (p = 0.0022) and treatment with exogenous high molecular weight HA (p = 0.0268) correlated with a significant decrease of HT1080 cell migration capacity. Transfection with siHAS2 and siHAS1 showed that mainly HAS1 synthesized high molecular weight HA regulates HT1080 cell motility. Induced degradation of the HA content by hyaluronidase treatment and addition of low molecular weight HA, resulted in a significant stimulation of HT1080 cells' motility (p < 0.01). In contrast, no effects on B6FS fibrosarcoma cell motility were observed.

Conclusions

bFGF regulates, in a cell-specific manner the migration capability of fibrosarcoma cells by modulating their HA metabolism.HA metabolism is suggested to be a potential therapeutic target in fibrosarcoma.
Keywords:HAS  hyaluronan synthase  HYAL  hyaluronidase  HA  hyaluronan  GAG  glycosaminoglycans  ECM  extracellular matrix  bFGF  basic fibroblast growth factor  RHAMM  Receptor for HA-Mediated Motility
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