Identify Non-mutational p53 Functional Deficiency in Human Cancers.

Qianpeng Li, Yang Zhang, Sicheng Luo, Zhang Zhang, Ann L Oberg, David E Kozono, Hua Lu, Jann N Sarkaria, Lina Ma, Liguo Wang
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Abstract

An accurate assessment of p53's functional status is critical for cancer genomic medicine. However, there is a significant challenge in identifying tumors with non-mutational p53 inactivations that are not detectable through DNA sequencing. These undetected cases are often misclassified as p53-normal, leading to inaccurate prognosis and downstream association analyses. To address this issue, we built the support vector machine (SVM) models to systematically reassess p53's functional status in TP53 wild-type (TP53  WT) tumors from multiple The Cancer Genome Atlas (TCGA) cohorts. Cross-validation demonstrated the good performance of the SVM models with a mean area under curve (AUC) of 0.9822, precision of 0.9747, and recall of 0.9784. Our study revealed that a significant proportion (87%-99%) of TP53  WT tumors actually have compromised p53 function. Additional analyses uncovered that these genetically intact but functionally impaired (termed as predictively reduced function of p53 or TP53  WT-pRF) tumors exhibited genomic and pathophysiologic features akin to TP53 mutant tumors: heightened genomic instability and elevated levels of hypoxia. Clinically, patients with TP53  WT-pRF tumors experienced significantly shortened overall survival or progression-free survival compared to those with predictively normal function of p53 (TP53  WT-pN) tumors, and these patients also displayed increased sensitivity to platinum-based chemotherapy and radiation therapy.

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确定人类癌症中的非突变 p53 功能缺陷。
准确评估 p53 的功能状态对癌症基因组医学至关重要。然而,如何识别无法通过 DNA 测序检测到的 p53 非突变失活的肿瘤是一项重大挑战。这些未检测到的病例往往被误判为 p53 正常,导致预后和下游关联分析不准确。为了解决这个问题,我们建立了支持向量机(SVM)模型,以系统地重新评估来自多个癌症基因组图谱(TCGA)队列的 TP53 野生型(TP53 WT)肿瘤中 p53 的功能状态。交叉验证表明 SVM 模型性能良好,平均曲线下面积 (AUC) 为 0.9822,精确度为 0.9747,召回率为 0.9784。我们的研究发现,相当大比例(87%-99%)的 TP53 WT 肿瘤实际上具有受损的 p53 功能。其他分析发现,这些基因完好但功能受损的肿瘤(称为预测性 p53 功能减退或 TP53 WT-pRF)表现出与 TP53 突变肿瘤相似的基因组和病理生理学特征:基因组不稳定性增强和缺氧水平升高。在临床上,与预测 p53 功能正常的肿瘤(TP53 WT-pN)相比,TP53 WT-pRF 肿瘤患者的总生存期或无进展生存期明显缩短,而且这些患者对铂类化疗和放疗的敏感性也有所提高。
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