Normann Lisa Svartdal, Haugen Mads Haugland, Aure Miriam Ragle, Kristensen Vessela N, Mælandsmo Gunhild Mari, Sahlberg Kristine Kleivi
Department of Research and Innovation, Vestre Viken Hospital Trust, Drammen, Norway.
Department of Tumor Biology, Institute for Cancer Research, Oslo University Hospital, Oslo, Norway.
Breast Cancer (Dove Med Press). 2022 Mar 1;14:25-39. doi: 10.2147/BCTT.S338404. eCollection 2022.
Human epidermal growth factor receptor 2 positive (HER2+) breast cancers responding poorly to targeted therapy need improved treatment options. miR-101-5p has shown tumor-suppressive properties in multiple cancer forms, and we assessed the effect and mechanism of action of this miRNA in HER2+ breast cancer.
Expression levels of miR-101-5p in two clinical datasets, TCGA and METABRIC, were compared between tumor and normal adjacent samples, and across molecular subtypes and HER2 status. The ability of miR-101-5p to sensitize for treatment with lapatinib, tucatinib and trastuzumab was explored in HER2+ breast cancer cells responding poorly to such targeted drugs. Proliferation and apoptosis assays and downstream protein analysis were performed.
Expression levels of miR-101-5p were significantly lower in tumor compared to normal adjacent tissue (p < 0.001), and particularly low in HER2+ tumors, both the HER2-enriched subtype (p ≤ 0.037) and clinical HER2-status (p < 0.001). In a HER2+ cell line (KPL4) responding poorly to targeted drugs, miR-101-5p overexpression inhibited proliferation (p < 0.001), and combinatorial treatment with lapatinib and trastuzumab significantly further decreased this inhibition (p = 0.004). Proteomic data and in silico analyses revealed PI3K/Akt- and HER2-pathways among the predicted regulated pathways. miR-101-5p alone (p = 0.018) and in combination with lapatinib and trastuzumab (p < 0.001) induced apoptosis, while the targeted drugs alone did not exert any significant effect neither on proliferation nor apoptosis.
miR-101-5p acts as a tumor suppressor by inducing apoptosis in HER2+ breast cancer and sensitizes cells with initially poor response to lapatinib and trastuzumab.
对靶向治疗反应不佳的人表皮生长因子受体2阳性(HER2+)乳腺癌需要更好的治疗选择。miR-101-5p在多种癌症类型中显示出肿瘤抑制特性,我们评估了这种微小RNA在HER2+乳腺癌中的作用效果及作用机制。
比较了肿瘤与相邻正常样本之间,以及不同分子亚型和HER2状态下,miR-101-5p在两个临床数据集(TCGA和METABRIC)中的表达水平。在对这类靶向药物反应不佳的HER2+乳腺癌细胞中,探究miR-101-5p对拉帕替尼、图卡替尼和曲妥珠单抗治疗的增敏作用。进行了增殖和凋亡检测以及下游蛋白分析。
与相邻正常组织相比,肿瘤组织中miR-101-5p的表达水平显著降低(p < 0.001),在HER2+肿瘤中尤其低,无论是HER2富集亚型(p≤0.037)还是临床HER2状态(p < 0.001)。在对靶向药物反应不佳的HER2+细胞系(KPL4)中,miR-101-5p过表达抑制增殖(p < 0.001),拉帕替尼和曲妥珠单抗联合治疗显著增强了这种抑制作用(p = 0.004)。蛋白质组学数据和计算机分析揭示PI3K/Akt和HER2通路是预测的受调控通路。单独的miR-101-5p(p = 0.018)以及与拉帕替尼和曲妥珠单抗联合使用(p < 0.001)均可诱导凋亡,而单独的靶向药物对增殖和凋亡均无显著影响。
miR-101-5p通过诱导HER2+乳腺癌细胞凋亡发挥肿瘤抑制作用,并使最初对拉帕替尼和曲妥珠单抗反应不佳的细胞增敏。
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