Khaleel Sari S, Andrews Erik H, Ung Matthew, DiRenzo James, Cheng Chao
Department of Genetics, Geisel School of Medicine at Dartmouth, 1 Rope Ferry Road, Hanover, NH, 03755, USA.
Department of Pharmacology & Toxicology, Geisel School of Medicine at Dartmouth, 1 Rope Ferry Road, Hanover, NH, 03755, USA.
Breast Cancer Res. 2014 Dec 2;16(6):486. doi: 10.1186/s13058-014-0486-7.
Genetic and molecular signatures have been incorporated into cancer prognosis prediction and treatment decisions with good success over the past decade. Clinically, these signatures are usually used in early-stage cancers to evaluate whether they require adjuvant therapy following surgical resection. A molecular signature that is prognostic across more clinical contexts would be a useful addition to current signatures.
We defined a signature for the ubiquitous tissue factor, E2F4, based on its shared target genes in multiple tissues. These target genes were identified by chromatin immunoprecipitation sequencing (ChIP-seq) experiments using a probabilistic method. We then computationally calculated the regulatory activity score (RAS) of E2F4 in cancer tissues, and examined how E2F4 RAS correlates with patient survival.
Genes in our E2F4 signature were 21-fold more likely to be correlated with breast cancer patient survival time compared to randomly selected genes. Using eight independent breast cancer datasets containing over 1,900 unique samples, we stratified patients into low and high E2F4 RAS groups. E2F4 activity stratification was highly predictive of patient outcome, and our results remained robust even when controlling for many factors including patient age, tumor size, grade, estrogen receptor (ER) status, lymph node (LN) status, whether the patient received adjuvant therapy, and the patient's other prognostic indices such as Adjuvant! and the Nottingham Prognostic Index scores. Furthermore, the fractions of samples with positive E2F4 RAS vary in different intrinsic breast cancer subtypes, consistent with the different survival profiles of these subtypes.
We defined a prognostic signature, the E2F4 regulatory activity score, and showed it to be significantly predictive of patient outcome in breast cancer regardless of treatment status and the states of many other clinicopathological variables. It can be used in conjunction with other breast cancer classification methods such as Oncotype DX to improve clinical outcome prediction.
在过去十年中,基因和分子特征已被纳入癌症预后预测和治疗决策,并取得了良好的成效。临床上,这些特征通常用于早期癌症,以评估手术切除后是否需要辅助治疗。一个在更多临床背景下具有预后价值的分子特征将是对当前特征的有益补充。
我们基于其在多个组织中的共享靶基因,为普遍存在的组织因子E2F4定义了一个特征。这些靶基因通过使用概率方法的染色质免疫沉淀测序(ChIP-seq)实验来鉴定。然后,我们通过计算得出癌症组织中E2F4的调控活性评分(RAS),并研究E2F4 RAS与患者生存率之间的相关性。
与随机选择的基因相比,我们的E2F4特征中的基因与乳腺癌患者生存时间相关的可能性高出21倍。使用包含超过1900个独特样本的八个独立乳腺癌数据集,我们将患者分为E2F4 RAS低分组和高分组。E2F4活性分层对患者预后具有高度预测性,即使在控制了许多因素后,我们的结果仍然稳健,这些因素包括患者年龄、肿瘤大小、分级、雌激素受体(ER)状态、淋巴结(LN)状态、患者是否接受辅助治疗以及患者的其他预后指标,如辅助治疗!和诺丁汉预后指数评分。此外, E2F4 RAS呈阳性的样本比例在不同的内在性乳腺癌亚型中有所不同,这与这些亚型的不同生存情况一致。
我们定义了一个预后特征,即E2F4调控活性评分,并表明它在乳腺癌患者预后预测中具有显著的预测能力,无论治疗状态以及许多其他临床病理变量的状态如何。它可以与其他乳腺癌分类方法(如Oncotype DX)结合使用,以改善临床预后预测。
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