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Modeling breast cancer progression to bone: how driver mutation order and metabolism matter

机译:模拟乳腺癌向骨骼的进展:驱动程序突变顺序和新陈代谢如何起作用

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摘要

BackgroundNot all the mutations are equally important for the development of metastasis. What about their order? The survival of cancer cells from the primary tumour site to the secondary seeding sites depends on the occurrence of very few driver mutations promoting oncogenic cell behaviours. Usually these driver mutations are among the most effective clinically actionable target markers. The quantitative evaluation of the effects of a mutation across primary and secondary sites is an important challenging problem that can lead to better predictability of cancer progression trajectory.
机译:背景并非所有的突变对于转移的发展都同样重要。他们的订单呢?癌细胞从原发肿瘤部位到继发接种部位的存活取决于促进致癌细胞行为的极少数驱动突变。通常,这些驱动程序突变是最有效的临床可操作靶标标记之一。对跨主要位点和次要位点的突变的影响进行定量评估是一个重要的挑战性问题,可导致癌症进展轨迹的更好可预测性。

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