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

AI Article Synopsis

  • This research suggests that features of normal wound healing are linked to cancer metastasis, highlighting consistent transcriptional responses in fibroblasts.
  • In a study of 295 early breast cancer patients, those with tumors showing a specific "wound-response signature" had significantly worse overall and distant metastasis-free survival compared to those without it.
  • The wound-response signature can provide a new prognostic score that enhances risk assessment, regardless of traditional clinical factors or existing prognosis models.

Article Abstract

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").

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC548329PMC
http://dx.doi.org/10.1073/pnas.0409462102DOI Listing

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