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首页> 外文期刊>Journal of molecular cell biology >Hunt for the tipping point during endocrine resistance process in breast cancer by dynamic network biomarkers
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Hunt for the tipping point during endocrine resistance process in breast cancer by dynamic network biomarkers

机译:通过动态网络生物标记物寻找乳腺癌内分泌抵抗过程中的临界点

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摘要

Acquired drug resistance is the major reason why patients fail to respond to cancer therapies. It is a challenging task to determine the tipping point of endocrine resistance and detect the associated molecules. Derived from new systems biology theory, the dynamic network biomarker (DNB) method is designed to quantitatively identify the tipping point of a drastic system transition and can theoretically identify DNB genes that play key roles in acquiring drug resistance. We analyzed time-course mRNA sequence data generated from the tamoxifen-treated estrogen receptor (ER)-positive MCF-7 cell line, and identified the tipping point of endocrine resistance with its leading molecules. The results show that there is interplay between gene mutations and DNB genes, in which the accumulated mutations eventually affect the DNB genes that subsequently cause the change of transcriptional landscape, enabling full-blown drug resistance. Survival analyses based on clinical datasets validated that the DNB genes were associated with the poor survival of breast cancer patients. The results provided the detection for the pre-resistance state or early signs of endocrine resistance. Our predictive method may greatly benefit the scheduling of treatments for complex diseases in which patients are exposed to considerably different drugs and may become drug resistant.
机译:获得性耐药是患者对癌症治疗无效的主要原因。确定内分泌抗性的临界点并检测相关分子是一项艰巨的任务。动态网络生物标记(DNB)方法源于新的系统生物学理论,旨在定量确定剧烈系统转换的临界点,并且理论上可以鉴定在获得耐药性中起关键作用的DNB基因。我们分析了由他莫昔芬治疗的雌激素受体(ER)阳性MCF-7细胞系产生的时程mRNA数据,并确定了其前导分子对内分泌抵抗的临界点。结果表明,基因突变与DNB基因之间存在相互作用,其中累积的突变最终影响DNB基因,随后引起转录景观的变化,从而实现了全面的耐药性。根据临床数据进行的生存分析证实,DNB基因与乳腺癌患者的不良生存能力有关。结果提供了对内分泌抵抗力的抵抗前状态或早期迹象的检测。我们的预测方法可能会大大有利于安排复杂疾病的治疗计划,在这些疾病中,患者会接触到截然不同的药物,并且可能会产生耐药性。

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