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Bone-in-culture array as a platform to model early-stage bone metastases and discover anti-metastasis therapies

机译:培养骨阵列作为模拟早期骨转移和发现抗转移疗法的平台

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摘要

The majority of breast cancer models for drug discovery are based on orthotopic or subcutaneous tumours. Therapeutic responses of metastases, especially microscopic metastases, are likely to differ from these tumours due to distinct cancer-microenvironment crosstalk in distant organs. Here, to recapitulate such differences, we established an ex vivo bone metastasis model, termed bone-in-culture array or BICA, by fragmenting mouse bones preloaded with breast cancer cells via intra-iliac artery injection. Cancer cells in BICA maintain features of in vivo bone micrometastases regarding the microenvironmental niche, gene expression profile, metastatic growth kinetics and therapeutic responses. Through a proof-of-principle drug screening using BICA, we found that danusertib, an inhibitor of the Aurora kinase family, preferentially inhibits bone micrometastases. In contrast, certain histone methyltransferase inhibitors stimulate metastatic outgrowth of indolent cancer cells, specifically in the bone. Thus, BICA can be used to investigate mechanisms involved in bone colonization and to rapidly test drug efficacies on bone micrometastases.
机译:大多数用于药物发现的乳腺癌模型均基于原位或皮下肿瘤。由于远处器官中明显的癌症-微环境串扰,转移瘤(尤其是微观转移瘤)的治疗反应可能与这些肿瘤有所不同。在这里,为了概括这种差异,我们通过碎片化通过-内动脉注射预加载了乳腺癌细胞的小鼠骨骼,建立了一种体外骨骼转移模型,称为骨培养阵列或BICA。 BICA中的癌细胞在微环境生态位,基因表达谱,转移性生长动力学和治疗反应方面保持体内骨骼微转移的特征。通过使用BICA的原则药物筛选,我们发现danusertib是Aurora激酶家族的一种抑制剂,可以优先抑制骨微转移。相反,某些组蛋白甲基转移酶抑制剂会刺激惰性癌细胞的转移性生长,特别是在骨骼中。因此,BICA可用于研究参与骨定植的机制,并快速测试药物对骨微转移的疗效。

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