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首页> 外文期刊>Cell death & disease. >Large-scale integrated analysis of ovarian cancer tumors and cell lines identifies an individualized gene expression signature for predicting response to platinum-based chemotherapy
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Large-scale integrated analysis of ovarian cancer tumors and cell lines identifies an individualized gene expression signature for predicting response to platinum-based chemotherapy

机译:卵巢癌肿瘤和细胞系的大规模综合分析鉴定了个体化基因表达签名,用于预测基于铂的化疗的反应

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摘要

Heterogeneity in chemotherapeutic response is directly associated with prognosis and disease recurrence in patients with ovarian cancer (OvCa). Despite the significant clinical need, a credible gene signature for predicting response to platinum-based chemotherapy and for guiding the selection of personalized chemotherapy regimens has not yet been identified. The present study used an integrated approach involving both OvCa tumors and cell lines to identify an individualized gene expression signature, denoted as IndividCRS, consisting of 16 robust chemotherapy-responsive genes for predicting intrinsic or acquired chemotherapy response in the meta-discovery dataset. The robust performance of this signature was subsequently validated in 25 independent tumor datasets comprising 2215 patients and one independent cell line dataset, across different technical platforms. The IndividCRS was significantly correlated with the response to platinum therapy and predicted the improved outcome. Moreover, the IndividCRS correlated with homologous recombination deficiency (HRD) and was also capable of discriminating HR-deficient tumors with or without platinum-sensitivity for guiding HRD-targeted clinical trials. Our results reveal the universality and simplicity of the IndividCRS as a promising individualized genomic tool to rapidly monitor response to chemotherapy and predict the outcome of patients with OvCa.
机译:化学治疗反应中的异质性与卵巢癌(OVCA)患者的预后和疾病复发直接相关。尽管临床需求重大,但尚未确定用于预测对基于铂类化疗和指导各种化疗方案的反应的可靠基因签名。本研究使用涉及OVCA肿瘤和细胞系的综合方法,以鉴定单个化的基因表达签名,其表示为单独的,由16种稳健的化疗响应基因组成,用于预测在Meta-Discovery DataSet中的内在或获得的化疗响应。随后在包括2215名患者和一个独立的细胞系数据集中的25个独立肿瘤数据集中验证了该签名的稳健性能。分类与对铂治疗的反应显着相关,并预测了改进的结果。此外,单独的分子与同源重组缺乏(HRD)相关,并且还能够区分具有或不具有铂敏感性的HR缺陷型肿瘤,用于引导HRD靶向临床试验。我们的结果揭示了个体化的普遍性和简单性,作为有前途的个性化的基因组工具,以便迅速监测化疗的反应,并预测OVCA患者的结果。

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