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Robustness, scalability, and integration of a wound-response gene expression signature in predicting breast cancer survival

机译:鲁棒性,可扩展性和伤口反应基因表达特征在预测乳腺癌存活率中的整合

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摘要

Based on the hypothesis that features of the molecular program of normal wound healing might play an important role in cancer metastasis, we previously identified consistent features in the transcriptional response of normal fibroblasts to serum, and used this "wound-response signature" to reveal links between wound healing and cancer progression in a variety of common epithelial tumors. Here, in a consecutive series of 295 early breast cancer patients, we show that both overall survival and distant metastasis-free survival are markedly diminished in patients whose tumors expressed this wound-response signature compared to tumors that did not express this signature. A gene expression centroid of the wound-response signature provides a basis for prospectively assigning a prognostic score that can be scaled to suit different clinical purposes. The wound-response signature improves risk stratification independently of known clinico-pathologic risk factors and previously established prognostic signatures based on unsupervised hierarchical clustering ("molecular subtypes") or supervised predictors of metastasis ("70-gene prognosis signature").
机译:基于正常伤口愈合分子程序的特征可能在癌症转移中起重要作用的假设,我们先前在正常成纤维细胞对血清的转录反应中鉴定出一致的特征,并使用这种“伤口反应特征”揭示了联系各种常见的上皮肿瘤中伤口愈合与癌症进展之间的关系。在此,在连续的295名早期乳腺癌患者中,我们发现与那些没有表达这种肿瘤的患者相比,那些表现出这种伤口反应特征的患者的总生存率和无远处转移的生存率均显着降低。伤口反应特征的基因表达重心为前瞻性分配预后评分提供了基础,该评分可缩放以适应不同的临床目的。伤口反应特征独立于已知的临床病理风险因素和先前基于无监督的分级聚类(“分子亚型”)或转移的有监督的预测因子(“ 70基因预后特征”)建立的预后特征,改善了危险分层。

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