Their progression along theosteogenic lineage and prevents apoptosis in more mature

Their progression along theosteogenic lineage and prevents apoptosis in more mature osteoblasts [4,5,6]. A role of Wnt signaling in osteosarcoma development is supported by the finding that several Wnt ligands, receptors and co-receptors are highly expressed while Wnt inhibitors are downregulated in osteosarcoma cells [7]. It was also shown that the Wnt inhibitory factor 1 is epigenetically silenced in human osteosarcoma, and its disruption accelerates osteosarcoma development in mice [8]. Hypericin web increased b-cateninmediated activity has been frequently reported in osteosarcoma [9,10,11], further supporting a role 1531364 for Wnt signaling in osteosarcoma development. The transcriptional cofactor LIM-only protein FHL2 (four and a half LIM domains protein 2) is a multifunctional adaptor protein that is involved in the regulation of signal transduction, gene expression, cell proliferation and differentiation [12,13]. The role of FHL2 in the development of cancers is complex. FHL2 was found to be down-regulated in some cancers and to be elevated in others compared to normal tissues, suggesting that FHL2 may act as an oncoprotein or a tumor suppressor, depending on its role as transcriptional activator or repressor in the cell type in which it isFHL2 Silencing Reduces Osteosarcoma Tumorigenesisexpressed [13]. One mechanism by which FHL2 may be linked to tumorigenesis is an interaction with key regulatory molecules. In muscle cells for example, FHL2 interacts with b-catenin and represses b-catenin-dependent transcription [14]. In contrast, in hepatoblastoma cells, FHL2 activates b-catenin-dependent transcription [15]. In bone, FHL2 was found to promote osteoblast differentiation [16,17,18]. We previously showed that FHL2 acts as an endogenous activator of mesenchymal cell differentiation into osteoblasts through its interaction with b-catenin and activation of Wnt/b-catenin signaling [19]. In these cells, overexpression of FHL2 increased Wnt/b-catenin signaling and osteogenic differentiation [19]. However, the implication of FHL2 in primary bone cancer progression and tumorigenesis has not been investigated. In this study, we used a shRNA-based technique to study the contribution of FHL2 in primary bone tumor cell growth, invasion and migration, and we used xenograft experiments in mice to analyse the impact of FHL2 on tumorigenesis in vivo. Our data indicate that FHL2 silencing reduces osteosarcoma cell tumorigenesis in vitro and in vivo, indicating that FHL2 is a potential target for therapeutical intervention in this type of cancer.Results FHL2 Expression is Expressed Above Normal in OsteosarcomaWe first analyzed by Western blot the expression of the FHL2 protein in a panel of human (U2OS, HOS, SaOS2, MG63) osteosarcoma cells with distinct genotypes compared to normal human osteoblasts (IHNC). We observed a single band at the predicted molecular weight in all cell lines tested (Fig. 1A). 1317923 FHL2 protein level was slightly increased in SaOS2 cells compared to normal cells, and was robustly expressed in MG63 and U2OS osteosarcoma cells. These results support the concept that FHL2 is expressed above normal in some human osteosarcoma cells in vitro. To determine the potential role of FHL2 in human osteosarcoma, we Argipressin chemical information investigated the expression of FHL2 in tissue microarray (TMA) from patients with osteosarcoma. Our immunohistochemical analysis showed that FHL2 was highly expressed in osteosarcoma tumors compared to normal bone (Fig. 1B). FHL2 expression tended to.Their progression along theosteogenic lineage and prevents apoptosis in more mature osteoblasts [4,5,6]. A role of Wnt signaling in osteosarcoma development is supported by the finding that several Wnt ligands, receptors and co-receptors are highly expressed while Wnt inhibitors are downregulated in osteosarcoma cells [7]. It was also shown that the Wnt inhibitory factor 1 is epigenetically silenced in human osteosarcoma, and its disruption accelerates osteosarcoma development in mice [8]. Increased b-cateninmediated activity has been frequently reported in osteosarcoma [9,10,11], further supporting a role 1531364 for Wnt signaling in osteosarcoma development. The transcriptional cofactor LIM-only protein FHL2 (four and a half LIM domains protein 2) is a multifunctional adaptor protein that is involved in the regulation of signal transduction, gene expression, cell proliferation and differentiation [12,13]. The role of FHL2 in the development of cancers is complex. FHL2 was found to be down-regulated in some cancers and to be elevated in others compared to normal tissues, suggesting that FHL2 may act as an oncoprotein or a tumor suppressor, depending on its role as transcriptional activator or repressor in the cell type in which it isFHL2 Silencing Reduces Osteosarcoma Tumorigenesisexpressed [13]. One mechanism by which FHL2 may be linked to tumorigenesis is an interaction with key regulatory molecules. In muscle cells for example, FHL2 interacts with b-catenin and represses b-catenin-dependent transcription [14]. In contrast, in hepatoblastoma cells, FHL2 activates b-catenin-dependent transcription [15]. In bone, FHL2 was found to promote osteoblast differentiation [16,17,18]. We previously showed that FHL2 acts as an endogenous activator of mesenchymal cell differentiation into osteoblasts through its interaction with b-catenin and activation of Wnt/b-catenin signaling [19]. In these cells, overexpression of FHL2 increased Wnt/b-catenin signaling and osteogenic differentiation [19]. However, the implication of FHL2 in primary bone cancer progression and tumorigenesis has not been investigated. In this study, we used a shRNA-based technique to study the contribution of FHL2 in primary bone tumor cell growth, invasion and migration, and we used xenograft experiments in mice to analyse the impact of FHL2 on tumorigenesis in vivo. Our data indicate that FHL2 silencing reduces osteosarcoma cell tumorigenesis in vitro and in vivo, indicating that FHL2 is a potential target for therapeutical intervention in this type of cancer.Results FHL2 Expression is Expressed Above Normal in OsteosarcomaWe first analyzed by Western blot the expression of the FHL2 protein in a panel of human (U2OS, HOS, SaOS2, MG63) osteosarcoma cells with distinct genotypes compared to normal human osteoblasts (IHNC). We observed a single band at the predicted molecular weight in all cell lines tested (Fig. 1A). 1317923 FHL2 protein level was slightly increased in SaOS2 cells compared to normal cells, and was robustly expressed in MG63 and U2OS osteosarcoma cells. These results support the concept that FHL2 is expressed above normal in some human osteosarcoma cells in vitro. To determine the potential role of FHL2 in human osteosarcoma, we investigated the expression of FHL2 in tissue microarray (TMA) from patients with osteosarcoma. Our immunohistochemical analysis showed that FHL2 was highly expressed in osteosarcoma tumors compared to normal bone (Fig. 1B). FHL2 expression tended to.