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胶质母细胞瘤异质性和可塑性的共调节影响图谱。

A coregulatory influence map of glioblastoma heterogeneity and plasticity.

作者信息

Bernhard Chloé, Geles Konstantinos, Pawlak Geoffrey, Dhifli Wajdi, Dispot Aurélien, Dusol Jules, Kondratova Maria, Martin Sophie, Messé Mélissa, Reita Damien, Tulasne David, Van Seuningen Isabelle, Entz-Werle Natacha, Ciafrè Silvia Anna, Dontenwill Monique, Elati Mohamed

机构信息

UMR7021 CNRS, University of Strasbourg, Illkirch, France.

Univ. Lille, CNRS, Inserm, CHU Lille, UMR9020-U1277 - CANTHER - Cancer Heterogeneity Plasticity and Resistance to Therapies, Lille, F-59000, France.

出版信息

NPJ Precis Oncol. 2025 Apr 15;9(1):110. doi: 10.1038/s41698-025-00890-0.

Abstract

We present GBM-cRegMap, an online resource providing a comprehensive coregulatory influence network perspective on glioblastoma (GBM) heterogeneity and plasticity. Using representation learning algorithms, we derived two components of this resource: GBM-CoRegNet, a highly specific coregulatory network of tumor cells, and GBM-CoRegMap, a unified network influence map based on 1612 tumors from 16 studies. As a widely applicable closed-loop system connecting cellular models and tumors, GBM-cRegMap will provide the GBM research community with an easy-to-use web tool ( https://gbm.cregmap.com ) that maps any existing or newly generated transcriptomic "query" data to a reference coregulatory network and a large-scale manifold of disease heterogeneity. Using GBM-cRegMap, we demonstrated the synergy between the two components by refining the molecular classification of GBM, identifying potential key regulators, and aligning the transcriptional profiles of tumors and in vitro models. Through the amalgamation of a vast dataset, we validated the proneural (PN)-mesenchymal (MES) axis and identified three subclasses of classical (CL) tumors: astrocyte-like (CL-A), epithelial basal-like (CL-B), and cilium-rich (CL-C). We revealed the CL-C subclass, an intermediate state demonstrating the plasticity of GBM cells along the PN-MES axis under chemotherapy. We identified key regulators, such as PAX8, and NKX2.5, potentially involved in temozolomide (TMZ) resistance. Notably, NKX2.5, more expressed in higher-grade gliomas, negatively impacts patient survival, and regulates genes involved in glucose metabolism.

摘要

我们展示了GBM-cRegMap,这是一个在线资源,它从综合的共调控影响网络角度呈现了胶质母细胞瘤(GBM)的异质性和可塑性。使用表征学习算法,我们得出了该资源的两个组成部分:GBM-CoRegNet,一个肿瘤细胞的高度特异性共调控网络,以及GBM-CoRegMap,一个基于16项研究中的1612个肿瘤的统一网络影响图谱。作为一个连接细胞模型和肿瘤的广泛适用的闭环系统,GBM-cRegMap将为GBM研究群体提供一个易于使用的网络工具(https://gbm.cregmap.com),该工具可将任何现有的或新生成的转录组“查询”数据映射到一个参考共调控网络以及一个大规模的疾病异质性流形上。使用GBM-cRegMap,我们通过完善GBM的分子分类、识别潜在的关键调控因子以及比对肿瘤和体外模型的转录谱,展示了这两个组成部分之间的协同作用。通过整合一个庞大的数据集,我们验证了神经前体细胞样(PN)-间充质细胞样(MES)轴,并识别出经典(CL)肿瘤的三个亚类:星形胶质细胞样(CL-A)、上皮基底样(CL-B)和富含纤毛(CL-C)。我们揭示了CL-C亚类,这是一种中间状态,表明GBM细胞在化疗下沿PN-MES轴具有可塑性。我们识别出了潜在参与替莫唑胺(TMZ)耐药性的关键调控因子,如PAX8和NKX2.5。值得注意的是,NKX2.5在高级别胶质瘤中表达更高,对患者生存有负面影响,并调控参与葡萄糖代谢的基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7571/12000621/3dbc4258c7fa/41698_2025_890_Fig1_HTML.jpg

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