Department of Pharmacy, Health and Nutritional Sciences, University of Calabria, 87036, Rende, Italy.
Breast Unit, Regional Hospital Cosenza, 87100, Cosenza, Italy.
J Transl Med. 2022 Jun 7;20(1):263. doi: 10.1186/s12967-022-03463-y.
Metabolic disorders are associated with increased incidence, aggressive phenotype and poor outcome of breast cancer (BC) patients. For instance, hyperinsulinemia is an independent risk factor for BC and the insulin/insulin receptor (IR) axis is involved in BC growth and metastasis. Of note, the anti-diabetic metformin may be considered in comprehensive therapeutic approaches in BC on the basis of its antiproliferative effects obtained in diverse pre-clinical and clinical studies.
Bioinformatics analysis were performed using the information provided by The Invasive Breast Cancer Cohort of The Cancer Genome Atlas (TCGA) project. The naturally immortalized BC cell line, named BCAHC-1, as well as cancer-associated fibroblasts (CAFs) derived from BC patients were used as model systems. In order to identify further mechanisms that characterize the anticancer action of metformin in BC, we performed gene expression and promoter studies as well as western blotting experiments. Moreover, cell cycle analysis, colony and spheroid formation, actin cytoskeleton reorganization, cell migration and matrigel drops evasion assays were carried out to provide novel insights on the anticancer properties of metformin.
We first assessed that elevated expression and activation of IR correlate with a worse prognostic outcome in estrogen receptor (ER)-positive BC. Thereafter, we established that metformin inhibits the insulin/IR-mediated activation of transduction pathways, gene changes and proliferative responses in BCAHC-1 cells. Then, we found that metformin interferes with the insulin-induced expression of the metastatic gene CXC chemokine receptor 4 (CXCR4), which we found to be associated with poor disease-free survival in BC patients exhibiting high levels of IR. Next, we ascertained that metformin prevents a motile phenotype of BCAHC-1 cells triggered by the paracrine liaison between tumor cells and CAFs upon insulin activated CXCL12/CXCR4 axis.
Our findings provide novel mechanistic insights regarding the anti-proliferative and anti-migratory effects of metformin in both BC cells and important components of the tumor microenvironment like CAFs. Further investigations are warranted to corroborate the anticancer action of metformin on the tumor mass toward the assessment of more comprehensive strategies halting BC progression, in particular in patients exhibiting metabolic disorders and altered insulin/IR functions.
代谢紊乱与乳腺癌(BC)患者发病率增加、侵袭性表型和预后不良有关。例如,高胰岛素血症是 BC 的独立危险因素,胰岛素/胰岛素受体(IR)轴参与 BC 的生长和转移。值得注意的是,基于在各种临床前和临床研究中观察到的抗增殖作用,二甲双胍这种抗糖尿病药物可能被考虑用于 BC 的综合治疗方法中。
使用癌症基因组图谱(TCGA)项目提供的信息进行了生物信息学分析。我们使用自然永生化的 BC 细胞系,命名为 BCAHC-1,以及来自 BC 患者的癌症相关成纤维细胞(CAFs)作为模型系统。为了进一步确定二甲双胍在 BC 中抗癌作用的特征机制,我们进行了基因表达和启动子研究以及 Western blot 实验。此外,还进行了细胞周期分析、集落和球体形成、肌动蛋白细胞骨架重排、细胞迁移和 Matrigel 滴逃避实验,以提供关于二甲双胍抗癌特性的新见解。
我们首先评估了 IR 的高表达和激活与雌激素受体(ER)阳性 BC 的预后不良相关。此后,我们确定二甲双胍抑制了 BCAHC-1 细胞中胰岛素/IR 介导的信号转导途径、基因变化和增殖反应的激活。然后,我们发现二甲双胍干扰了胰岛素诱导的转移性基因 CXC 趋化因子受体 4(CXCR4)的表达,我们发现,在 IR 水平高的 BC 患者中,CXCR4 的表达与无病生存期差相关。接下来,我们确定二甲双胍阻止了由肿瘤细胞和 CAFs 之间的旁分泌联系触发的 BCAHC-1 细胞的迁移表型,该联系是由胰岛素激活的 CXCL12/CXCR4 轴引发的。
我们的研究结果为二甲双胍在 BC 细胞以及肿瘤微环境中的重要组成部分(如 CAFs)中的抗增殖和抗迁移作用提供了新的机制见解。需要进一步的研究来证实二甲双胍对肿瘤的抗癌作用,以评估阻止 BC 进展的更全面的策略,特别是在存在代谢紊乱和胰岛素/IR 功能改变的患者中。
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