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对患者来源的卵巢癌模型进行综合分子分析,确定具有临床相关性的特征和肿瘤易损性。

Integrated molecular profiling of patient-derived ovarian cancer models identifies clinically relevant signatures and tumor vulnerabilities.

机构信息

Unit of Gynaecological Oncology Research, European Institute of Oncology IRCCS, Milan, Italy.

Unit of Cancer Biomarkers, Fondazione IRCCS Casa Sollievo della Sofferenza, San Giovanni Rotondo, Italy.

出版信息

Int J Cancer. 2022 Jul 15;151(2):240-254. doi: 10.1002/ijc.33983. Epub 2022 Mar 14.

Abstract

High-grade serous ovarian carcinoma (HGSOC) is a highly aggressive and intractable neoplasm, mainly because of its rapid dissemination into the abdominal cavity, a process that is favored by tumor-associated peritoneal ascites. The precise molecular alterations involved in HGSOC onset and progression remain largely unknown due to the high biological and genetic heterogeneity of this tumor. We established a set of different tumor samples (termed the As11-set) derived from a single HGSOC patient, consisting of peritoneal ascites, primary tumor cells, ovarian cancer stem cells (OCSC) and serially propagated tumor xenografts. The As11-set was subjected to an integrated RNA-seq and DNA-seq analysis which unveiled molecular alterations that marked the different types of samples. Our profiling strategy yielded a panel of signatures relevant in HGSOC and in OCSC biology. When such signatures were used to interrogate the TCGA dataset from HGSOC patients, they exhibited prognostic and predictive power. The molecular alterations also identified potential vulnerabilities associated with OCSC, which were then tested functionally in stemness-related assays. As a proof of concept, we defined PI3K signaling as a novel druggable target in OCSC.

摘要

高级别浆液性卵巢癌(HGSOC)是一种高度侵袭性和难治性肿瘤,主要是因为其在腹腔内迅速扩散,这一过程受到肿瘤相关腹膜腹水的影响。由于这种肿瘤具有高度的生物学和遗传异质性,HGSOC 发病和进展的确切分子改变在很大程度上仍然未知。我们建立了一组源自单个 HGSOC 患者的不同肿瘤样本(称为 As11 集),包括腹膜腹水、原代肿瘤细胞、卵巢癌干细胞(OCSC)和连续传代的肿瘤异种移植物。对 As11 集进行了整合的 RNA-seq 和 DNA-seq 分析,揭示了标记不同类型样本的分子改变。我们的分析策略产生了一组与 HGSOC 和 OCSC 生物学相关的特征。当将这些特征用于分析来自 HGSOC 患者的 TCGA 数据集时,它们表现出了预后和预测能力。这些分子改变还确定了与 OCSC 相关的潜在弱点,然后在与干细胞相关的测定中对其进行了功能测试。作为概念验证,我们将 PI3K 信号定义为 OCSC 中的一个新的可用药靶。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8856/9310611/69803ae2d007/IJC-151-240-g002.jpg

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