Cifuentes Claudia, Horndler Lydia, Grosso Pilar, Oeste Clara L, Hortal Alejandro M, Castillo Jennifer, Fernández-Pisonero Isabel, Paradela Alberto, Bustelo Xosé, Alarcón Balbino
Immune System Development and Function Program, Centro Biología Molecular Severo Ochoa, Consejo Superior de Investigaciones Científicas, Universidad Autónoma de Madrid, Madrid, 28049, Spain.
Savana, S.L., Calle Gran Vía 30, Madrid, 28013, Spain.
J Hematol Oncol. 2025 Apr 12;18(1):41. doi: 10.1186/s13045-025-01693-3.
Recent research from our group has shown that the overexpression of the wild-type RAS-family GTPase RRAS2 drives the onset of triple-negative breast cancer (TNBC) in mice following one or more pregnancies. This phenomenon mirrors human TNBC, where RRAS2 is overexpressed in approximately 75% of cases, particularly in tumors associated with the postpartum period. These findings underscore the relevance of R-RAS2 in TNBC development and progression.
We conducted RNA sequencing on tumors derived from conditional knock-in mice overexpressing human wild-type RRAS2 to identify the somatic mutation landscape associated with TNBC development in these mice. Additionally, we developed a TNBC cell line from RRAS2-overexpressing mice, enabling loss-of-function studies to investigate the role of R-RAS2 in various pathobiological parameters of TNBC cells, including cell migration, invasiveness, metabolic activity, and metastatic spread. Furthermore, proteomic analysis of a freshly isolated tumor identified plasma membrane receptors interacting with R-RAS2.
Our findings demonstrate that TNBC driven by RRAS2 overexpression exhibits a pattern of somatic mutations similar to those observed in human breast cancer, particularly in genes involved in stemness, extracellular matrix interactions, and actin cytoskeleton regulation. Proteomic analysis revealed that wild-type R-RAS2 interacts with 245 membrane-associated proteins, including key solute carriers involved in cell metabolism (CD98/LAT1, GLUT1, and basigin), adhesion and matrix interaction proteins (CD44, EpCAM, MCAM, ICAM1, integrin-α6, and integrin-β1), and stem cell markers (β1-catenin, α1-catenin, PTK7, and CD44). We show that R-RAS2 regulates CD98/LAT1 transporter-mediated mTOR pathway activation and mediates CD44-dependent cancer cell migration and invasion, thus providing a mechanism by which R-RAS2 promotes breast cancer cell metastasis.
R-RAS2 associates with CD44, CD98/LAT1, and other plasma membrane receptors to regulate metabolic activity, actin cytoskeleton reorganization, cell migration, invasion, and distant metastasis formation in TNBC. These findings establish R-RAS2 as a central driver of TNBC malignancy and highlight its potential as a promising therapeutic target, particularly in aggressive, postpartum-associated breast cancers.
我们团队最近的研究表明,野生型RAS家族GTP酶RRAS2的过表达会在小鼠经历一次或多次怀孕后引发三阴性乳腺癌(TNBC)。这种现象与人类TNBC相似,在大约75%的病例中RRAS2过表达,特别是在与产后时期相关的肿瘤中。这些发现强调了R-RAS2在TNBC发生和发展中的相关性。
我们对来自过表达人类野生型RRAS2的条件性敲入小鼠的肿瘤进行了RNA测序,以确定与这些小鼠TNBC发生相关的体细胞突变图谱。此外,我们从RRAS2过表达小鼠中建立了一个TNBC细胞系,从而能够进行功能缺失研究,以探讨R-RAS2在TNBC细胞的各种病理生物学参数中的作用,包括细胞迁移、侵袭性、代谢活性和转移扩散。此外,对新鲜分离的肿瘤进行蛋白质组分析,确定了与R-RAS2相互作用的质膜受体。
我们的研究结果表明,由RRAS2过表达驱动的TNBC表现出与人类乳腺癌相似的体细胞突变模式,特别是在涉及干性、细胞外基质相互作用和肌动蛋白细胞骨架调节的基因中。蛋白质组分析显示,野生型R-RAS2与245种膜相关蛋白相互作用,包括参与细胞代谢的关键溶质载体(CD98/LAT1、GLUT1和基底膜蛋白)、黏附与基质相互作用蛋白(CD44、EpCAM、MCAM、ICAM1、整合素-α6和整合素-β1)以及干细胞标志物(β-连环蛋白、α-连环蛋白、PTK7和CD44)。我们表明,R-RAS2调节CD98/LAT1转运体介导的mTOR途径激活,并介导CD44依赖性癌细胞迁移和侵袭,从而提供了一种R-RAS2促进乳腺癌细胞转移的机制。
R-RAS2与CD44、CD98/LAT1和其他质膜受体相关联,以调节TNBC中的代谢活性、肌动蛋白细胞骨架重组、细胞迁移、侵袭和远处转移形成。这些发现确立了R-RAS2作为TNBC恶性肿瘤的核心驱动因素,并突出了其作为有前景的治疗靶点的潜力,特别是在侵袭性、产后相关乳腺癌中。
Zotero 插件
