Guo Guang-Cheng, Wang Jia-Xiang, Han Ming-Li, Zhang Lian-Ping, Li Lin
Department of Breast Surgery, The First Affiliated Hospital of Zhengzhou University, Zhengzhou, China.
Cell Oncol (Dordr). 2017 Apr;40(2):157-166. doi: 10.1007/s13402-016-0312-6. Epub 2017 Jan 4.
Despite advances that have been made in systemic chemotherapy, the prognosis of advanced triple-negative breast cancer (TNBC) patients is still poor. The identification of key factors governing TNBC development is considered imperative for the development of novel effective therapeutic approaches. Previously, it has been reported that microRNA (miR)-761 may act as either a tumor suppressor or as an oncogene in different types of cancer. Here, we aimed at assessing the biological role of this miRNA in TNBC.
First, we measured the expression of miR-761 in primary breast cancer tissues and breast cancer-derived cell lines using qRT-PCR. Subsequently, over-expression and silencing experiments were performed to determine the role of miR-761 in TNBC cell proliferation, colony formation, migration and invasion in vitro. The in vivo role of miR-761 in TNBC growth and metastasis was determined in mouse models. Bioinformatics analyses, dual-luciferase reporter assays, Western blot analyses and rescue experiments were performed to identify miR-761 target gene(s).
We found that miR-761 was up-regulated in primary breast cancer tissues and its derived cell lines and, particularly, in TNBC tissues and cell lines. We also found that exogenous miR-761 over-expression augmented in vitro TNBC cell proliferation, colony formation, migration and invasion, whereas miR-761 down-regulation impaired these features. In vivo, we found that miR-761 over-expression facilitated TNBC growth and lung metastasis. Mechanistically, miR-761 was found to negatively regulate the expression of tripartite motif-containing 29 (TRIM29) in TNBC cells by binding to the 3'-untranslated region of its mRNA. In conformity with these results, a significant negative correlation between miR-761 expression and TRIM29 protein expression was noted in primary TNBC tissues (r = -0.452, p = 0.0126). We also found that exogenous TRIM29 over-expression reversed the proliferative and invasive capacities of TNBC cells.
Our data indicate that miR-761 acts as an oncogene in TNBC. This mode of action can, at least partially, be ascribed to the down-regulation of its target TRIM29. We suggest that miR-761 may serve as a promising therapeutic target for TNBC.
尽管全身化疗已取得进展,但晚期三阴性乳腺癌(TNBC)患者的预后仍然很差。确定TNBC发展的关键因素被认为是开发新型有效治疗方法的必要条件。此前,有报道称微小RNA(miR)-761在不同类型的癌症中可能作为肿瘤抑制因子或癌基因发挥作用。在此,我们旨在评估这种miRNA在TNBC中的生物学作用。
首先,我们使用qRT-PCR检测了原发性乳腺癌组织和乳腺癌衍生细胞系中miR-761的表达。随后,进行了过表达和沉默实验,以确定miR-761在体外TNBC细胞增殖、集落形成、迁移和侵袭中的作用。在小鼠模型中确定了miR-761在TNBC生长和转移中的体内作用。进行了生物信息学分析、双荧光素酶报告基因检测、蛋白质免疫印迹分析和拯救实验,以鉴定miR-761的靶基因。
我们发现miR-761在原发性乳腺癌组织及其衍生细胞系中上调,尤其是在TNBC组织和细胞系中。我们还发现,外源性miR-761过表达增强了体外TNBC细胞的增殖、集落形成、迁移和侵袭,而miR-761下调则损害了这些特性。在体内,我们发现miR-761过表达促进了TNBC的生长和肺转移。机制上,发现miR-761通过与其mRNA的3'非翻译区结合来负调节TNBC细胞中含三联体基序的29(TRIM29)的表达。与这些结果一致,在原发性TNBC组织中观察到miR-761表达与TRIM29蛋白表达之间存在显著负相关(r = -0.452,p = 0.0126)。我们还发现,外源性TRIM29过表达逆转了TNBC细胞的增殖和侵袭能力。
我们的数据表明miR-761在TNBC中作为癌基因发挥作用。这种作用模式至少部分可归因于其靶标TRIM29的下调。我们建议miR-761可能成为TNBC的一个有前景的治疗靶点。
