Comparative responses to demethylating therapy in animal models of osteosarcoma.

Shan Huang, Ling Ren, Jessica A Beck, Sushant Patkar, Maria Angeles Lillo Osuna, Aswini Cherukuri, Christina Mazcko, Susan A Krum, Amy K LeBlanc
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Abstract

Background: The demethylating agent decitabine (DAC) effectively inhibits tumor growth and metastasis by targeting ESR1 methylation to restore estrogen receptor alpha (ERα) signaling and promoting cellular differentiation in models of human osteosarcoma (OSA). Whether this pathway can be targeted in canine OSA patients is unknown.

Methods: Canine OSA tumor samples were tested for ERα expression and ESR1 promoter methylation. Human (MG63.3) and canine (MC-KOS) OSA cell lines and murine xenografts were treated with DAC in vitro and in vivo, respectively. Samples were assessed using mRNA sequencing and tissue immunohistochemistry.

Results: ESR1 is methylated in a subset of canine OSA patient samples and the MC-KOS cell line. DAC treatment led to enhanced differentiation as demonstrated by increased ALPL expression, and suppressed tumor growth in vitro and in vivo. Metastatic progression was inhibited, particularly in the MG63.3 model, which expresses higher levels of DNA methyltransferases DNMT1 and 3B. DAC treatment induced significant alterations in immune response and cell cycle pathways.

Conclusion: DAC treatment activates ERα signaling, promotes bone differentiation, and inhibits tumor growth and metastasis in human and canine OSA. Additional DAC-altered pathways and species- or individual-specific differences in DNMT expression may also play a role in DAC treatment of OSA.

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骨肉瘤动物模型对去甲基化疗法的比较反应。
背景 在人类骨肉瘤(OSA)模型中,去甲基化剂地西他滨(DAC)通过靶向 ESR1 甲基化来恢复雌激素受体α(ERα)信号传导,促进细胞分化,从而有效抑制肿瘤生长和转移。犬 OSA 患者是否也能以这一途径为靶点尚不清楚。方法 对犬 OSA 肿瘤样本进行 ERα 表达和 ESR1 启动子甲基化检测。分别在体外和体内用 DAC 处理人(MG63.3)和犬(MC-KOS)OSA 细胞系和鼠异种移植物。使用 mRNA 测序和组织免疫组化对样本进行评估。结果 在一部分犬 OSA 患者样本和 MC-KOS 细胞系中,ESR1 被甲基化。DAC 处理可增强分化(表现为 ALPL 表达增加),并抑制肿瘤在体外和体内的生长。转移进展受到抑制,尤其是在 DNA 甲基转移酶 DNMT1 和 3B 表达水平较高的 MG63.3 模型中。DAC 治疗诱导免疫反应和细胞周期通路发生显著变化。结论 DAC 治疗可激活 ERα 信号传导,促进骨分化,抑制人类和犬 OSA 的肿瘤生长和转移。DAC改变的其他通路以及物种或个体特异性的DNMT表达差异也可能在DAC治疗OSA中发挥作用。
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