Oncostatin M Induces Bone Loss and Sensitizes Rat Osteosarcoma to the Antitumor Effect of Midostaurin<i>In vivo</i>

Histone modifications are important for maintaining the transcription program. BET proteins, an important class of "histone reading proteins", have recently been described as essential in bone biology. This study presents the therapeutic opportunity of BET protein inhibition in osteoporosis. We find that the pharmacological BET protein inhibitor JQ1 rescues pathologic bone loss in a post-ovariectomy osteoporosis model by increasing the trabecular bone volume and restoring mechanical properties. The BET protein inhibition suppresses osteoclast differentiation and activity as well as the osteoblastogenesis in vitro. Moreover, we show that treated non-resorbing osteoclasts could still activate osteoblast differentiation. In addition, specific inhibition of BRD4 using RNA interference inhibits osteoclast differentiation but strongly activates osteoblast mineralization activity. Mechanistically, JQ1 inhibits expression of the master osteoclast transcription factor NFATc1 and the transcription factor of osteoblast Runx2. These findings strongly support that targeting epigenetic chromatin regulators such as BET proteins may offer a promising alternative for the treatment of bone-related disorders such as osteoporosis.

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“…Sections (3 m thick, Leica Microsystems) were analyzed by tartrate-resistant acid phosphatase (TRAP) staining as described previously [17,18].…”

Section: Bone Histomorphometric Analysismentioning

confidence: 99%

“…Immunostaining for Osterix was performed as described [17] For undecalcified histology, tibias were methylmethacrylate-embedded for microtome sectioning (6 m) for von Kossa staining.…”

Section: Bone Histomorphometric Analysismentioning

confidence: 99%

Inhibition of BET proteins and epigenetic signaling as a potential treatment for osteoporosis

Baud’huin

Lamoureux

Jacques

et al. 2017

Bone

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“…The tumor volume was quantified by measuring two perpendicular diameters with a vernier caliper and calculated with the formula: (l 2 Â L)/2 (l, the smallest and L, the largest diameter). 29,34 In-vivo treatment with Adenovirus Replication-deficient adenovirus encoding mouse OSM (AdOSM) has been described previously 29,36 and was produced, together with adenovirus encoding green fluorescent protein (AdGFP), in the vector facility of the INSERM U649 Laboratory (Nantes, France). Approximately 20 days after transplantation when tumor volumes reached 1,000 mm 3 (considered as progressive tumors), rats were injected at three points in the tumor with either PBS, AdOSM or AdGFP at a dose of 1.10 9 pfu.…”

Section: Experimental Chondrosarcoma Modelmentioning

confidence: 99%

“…15,28 However, OSM or IL-6 block osteoblasts and osteosarcoma cells in the G0/G1 phase of the cell cycle by inducing expression of the cdk inhibitor p21 WAF1 . 17,29,30 These cytokines do not induce apoptosis, but wild-type p53 osteosarcoma cells treated with OSM are particularly sensitive to apoptosis induced by staurosporine (STS), UV, TNFa or chemotherapeutic agents. 29,31 Indeed OSM, through activation of STATs and p53, increases the Bax/Bcl2 ratio which controls the mitochondrial apoptotic pathway.…”

mentioning

confidence: 99%

“…17,29,30 These cytokines do not induce apoptosis, but wild-type p53 osteosarcoma cells treated with OSM are particularly sensitive to apoptosis induced by staurosporine (STS), UV, TNFa or chemotherapeutic agents. 29,31 Indeed OSM, through activation of STATs and p53, increases the Bax/Bcl2 ratio which controls the mitochondrial apoptotic pathway. 31 These effects on cell proliferation and apoptosis are concomitant with an induced terminal differentiation of osteoblasts or osteosarcoma cells into osteocyte-like cells.…”

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confidence: 99%

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Direct anti‐cancer effect of oncostatin M on chondrosarcoma

David

Guihard

Brounais

et al. 2011

Intl Journal of Cancer

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The cytokine Oncostatin M (OSM) is cytostatic, pro-apoptotic and induces differentiation of osteosarcoma cells into osteocytes, suggesting new adjuvant treatment for these bone-forming sarcomas. However, OSM systemic over-expression could lead to adverse side effects such as generalized inflammation, neoangiogenesis and osteolysis. We determine here the effect of OSM on chondrosarcoma, another primary bone sarcoma characterized by the production of cartilage matrix and altered bone remodelling. Chondrosarcomas are resistant to conventional chemotherapy and radiotherapy, and wide surgical excision remains the only available treatment. We found that OSM blocked the cell cycle in four of five chondrosarcoma cell lines, independently of p53 and presumably through the JAK3/STAT1 pathway. In two tested cell lines, OSM induced a hypertrophic chondrocyte differentiation, with an induced Cbfa1/SOX9 ratio and induced Coll10, matrix metalloproteinase 13 (MMP13) and RANKL expression. Adenoviral gene transfer of OSM (AdOSM) in the Swarm rat chondrosarcoma (SRC) model indicated that local intra-tumoral OSM over-expression reduces chondrosarcoma development not only with reduced tumor proliferation and enhanced apoptosis but also with enhanced RANKL expression, osteoclast formation and reduced bone volumes. Flu-like symptoms were induced by the AdOSM, but there was no effect on tumor angiogenesis. Therefore, OSM could be considered as a new adjuvant anti-cancer agent for chondrosarcomas. A local application of this cytokine is presumably needed to overcome the poor vascularization of these tumors and to limit the deleterious effect on other tissues. Its side effect on bone remodeling could be managed with anti-resorption agents, thus offering potential new lines of therapeutic interventions.

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The multikinase inhibitor EC‐70124 synergistically increased the antitumor activity of doxorubicin in sarcomas

Estupiñán

Santos

Rodríguez

et al. 2019

Intl Journal of Cancer

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Cytotoxic drugs like doxorubicin remain as the most utilized agents in sarcoma treatment. However, advanced sarcomas are often resistant, thus stressing the need for new therapies aimed to overcome this resistance. Multikinase inhibitors provide an efficient way to target several pro‐tumorigenic pathways using a single agent and may constitute a valuable strategy in the treatment of sarcomas, which frequently show an aberrant activation of pro‐tumoral kinases. Therefore, we studied the antitumor activity of EC‐70124, an indolocarbazole analog that have demonstrated a robust ability to inhibit a wide range of pro‐survival kinases. Evaluation of the phospho‐kinase profile in cell‐of‐origin sarcoma models and/or sarcoma primary cell lines evidenced that PI3K/AKT/mTOR, JAK/STAT or SRC were among the most highly activated pathways. In striking contrast with the structurally related drug midostaurin, EC‐70124 efficiently prevented the phosphorylation of these targets and robustly inhibited proliferation through a mechanism associated to the induction of DNA damage, cell cycle arrest and apoptosis. In addition, EC‐70124 was able to partially reduce tumor growth in vivo. Importantly, this compound inhibited the expression and activity of ABC efflux pumps involved in drug resistance. In line with this ability, we found that the combined treatment of EC‐70124 with doxorubicin resulted in a synergistic cytotoxic effect in vitro and an increased antitumor activity of this cytotoxic drug in vivo. Altogether, these results uncover the capability of the novel multikinase inhibitor EC‐70124 to counteract drug resistance in sarcoma and highlight its therapeutic potential when combined with current treatments.

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Oncostatin M Induces Bone Loss and Sensitizes Rat Osteosarcoma to the Antitumor Effect of MidostaurinIn vivo

Cited by 33 publications

References 41 publications

Inhibition of BET proteins and epigenetic signaling as a potential treatment for osteoporosis

Inhibition of BET proteins and epigenetic signaling as a potential treatment for osteoporosis

Direct anti‐cancer effect of oncostatin M on chondrosarcoma

The multikinase inhibitor EC‐70124 synergistically increased the antitumor activity of doxorubicin in sarcomas

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