ELK1 在调控结直肠癌进展中的作用:miR-31-5p/CDIP1 轴在 CRC 发病机制中的作用。
Role of ELK1 in regulating colorectal cancer progression: miR-31-5p/CDIP1 axis in CRC pathogenesis.
机构信息
Department of Colorectal & Anal Surgery, The First Hospital of Jilin University, Changchun, Jilin, China.
出版信息
PeerJ. 2023 Jul 31;11:e15602. doi: 10.7717/peerj.15602. eCollection 2023.
BACKGROUND AND OBJECTIVE
Colorectal cancer (CRC) is a malignant tumor that affects the digestive system. With the increased of modernization of society, the incidence of colorectal cancer has increased throughout the world. As a transcription factor, ELK1 has been widely studied in colorectal cancer. However, there are still many unknown factors regarding its specific mechanism of action.This study explored the role of ELK1 and its downstream pathway in CRC pathogenesis.
METHODS
Based on clinical samples, this study examined miR-31-5p expression in CRC cells and its impact on malignant behaviors (migration, invasion, apoptosis) and autophagy. The promoter sequence of miR-31-5p was obtained from the UCSC database, and ELK1 was identified as its transcription factor. In ELK1-knockdown CRC cells, miR-31-5p was overexpressed, and its response in malignant behaviors and autophagy was analyzed. The target gene CDIP1 was predicted and verified using a dual-luciferase assay. The influence of CDIP1 on malignant behavior in CRC cells was assessed, and CDIP1 siRNA was used as a rescue treatment for miR-31-5p inhibition. The role of ELK1/miR-31-5p in tumor growth was validated .
RESULTS
miR-31-5p expression was upregulated in the colorectal cancer tissues and cells. The knockdown of miR-31-5p markedly inhibited cancer cells' malignant behaviors and mediated autophagy. ELK1 was confirmed to bind with the miR-31-5p promoter and enhance miR-31-5p transcription. miR-31-5p was found to bind with the CDIP1 3'UTR and inhibit CDIP1 expression. CDIP1 siRNA partially rescued the effects of miR-31-5p knockdown on cell metastatic ability, autophagy, and apoptosis. Based on the experiments, results showed that the ELK1/miR-31-5p axis positively regulated tumor growth in nude mice.
CONCLUSION
Our findings indicate that ELK1 regulates the progression of colorectal cancer an miR-31-5p/CDIP1 axis, and the ELK1/miR-31-5p/CDIP1 axis could be a therapeutic target for colorectal cancer.
背景与目的
结直肠癌(CRC)是一种影响消化系统的恶性肿瘤。随着社会现代化程度的提高,CRC 的全球发病率一直在上升。作为一种转录因子,ELK1 在结直肠癌中得到了广泛的研究。然而,其具体作用机制仍有许多未知因素。本研究探讨了 ELK1 及其下游通路在 CRC 发病机制中的作用。
方法
本研究基于临床样本,检测了结直肠癌细胞中 miR-31-5p 的表达及其对恶性行为(迁移、侵袭、凋亡)和自噬的影响。从 UCSC 数据库中获得 miR-31-5p 的启动子序列,并鉴定 ELK1 为其转录因子。在 ELK1 敲低的 CRC 细胞中过表达 miR-31-5p,分析其对恶性行为和自噬的反应。利用双荧光素酶报告基因实验预测和验证 CDIP1 为其靶基因。评估 CDIP1 对 CRC 细胞恶性行为的影响,并采用 CDIP1 siRNA 进行抑制 miR-31-5p 后的挽救治疗。验证 ELK1/miR-31-5p 对肿瘤生长的作用。
结果
miR-31-5p 在结直肠癌组织和细胞中表达上调。抑制 miR-31-5p 的表达显著抑制了癌细胞的恶性行为,并介导了自噬。证实 ELK1 与 miR-31-5p 启动子结合,增强了 miR-31-5p 的转录。发现 miR-31-5p 与 CDIP1 3'UTR 结合,抑制 CDIP1 的表达。CDIP1 siRNA 部分挽救了 miR-31-5p 敲低对细胞转移能力、自噬和凋亡的影响。基于这些实验结果表明,ELK1/miR-31-5p 轴正向调控裸鼠肿瘤生长。
结论
本研究结果表明,ELK1 通过 miR-31-5p/CDIP1 轴调控结直肠癌的进展,ELK1/miR-31-5p/CDIP1 轴可能成为结直肠癌的治疗靶点。
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