长链非编码RNA DUXAP8通过微小RNA-378a-3p/FOXQ1轴促进结肠癌的恶性进展。

The Long Noncoding RNA DUXAP8 Facilitates the Malignant Progression of Colon Cancer via the microRNA-378a-3p/FOXQ1 Axis.

作者信息

Shang Rui, Jin Jianqin, Wang Yuecheng

机构信息

Department of Gastroenterology, Renmin Hospital, Hubei University of Medicine, Shiyan, China.

出版信息

Gut Liver. 2025 Mar 15;19(2):219-235. doi: 10.5009/gnl240178. Epub 2024 Nov 20.

DOI:10.5009/gnl240178

PMID:39563395

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11907261/

Abstract

BACKGROUND/AIMS: The long noncoding RNA DUXAP8 is a pivotal regulator in cancer pathogenesis, but the molecular mechanism underlying the role of DUXAP8 in colon cancer progression is underexplored.

METHODS

In addition to bioinformatic analyses, quantitative reverse transcription polymerase chain reaction (qRT-PCR) was performed to assess DUXAP8, microRNA-378a-3p, FOXQ1 expression in colon cancer tissues, and clinical data were analyzed to determine the correlation between DUXAP8 expression and colon cancer patient outcomes. Nuclear/cytoplasmic RNA fractionation was utilized to analyze the subcellular distribution of DUXAP8. Dual-luciferase and RNA immunoprecipitation assays were performed to confirm the binding of DUXAP8/FOXQ1 and microRNA-378a-3p. After cell transfection, qRT-PCR was performed to evaluate the modulatory relationship of DUXAP8/microRNA-378a-3p/FOXQ1. Cell Counting Kit-8, MTT, scratch healing, and Transwell assays were performed to evaluate the impact of DUXAP8/microRNA-378a-3p/FOXQ1 expression on colon cancer cell functions.

RESULTS

The results revealed that the expression of DUXAP8 and FOXQ1 was upregulated in colon cancer tissues, while the expression of microRNA-378a-3p was down-regulated. The increased DUXAP8 expression was positively correlated with lymph node metastasis and TNM stage. Dual-luciferase and RNA immunoprecipitation assays demonstrated that DUXAP8 was a sponge for microRNA-378a-3p and targeted the ability of microRNA-378a-3p to regulate FOXQ1. In addition, functional experiment results revealed that overexpressed DUXAP8 facilitated the growth and migratory ability of colon cancer cells. DUXAP8 also reversed the tumor-suppressive effect of microRNA-378a-3p. However, silencing FOXQ1 could reverse the cancer-promoting effects of high DUXAP8 expression.

CONCLUSIONS

DUXAP8 expression was significantly increased in colon cancer, which was associated with lymph node metastasis and unfavorable outcomes in colon cancer patients. DUXAP8 may hasten malignant progression of colon cancer cells through its effects on microRNA-378a-3p/FOXQ1.

摘要

背景/目的：长链非编码RNA DUXAP8是癌症发病机制中的关键调节因子，但DUXAP8在结肠癌进展中作用的分子机制尚未得到充分研究。

方法

除生物信息学分析外，采用定量逆转录聚合酶链反应（qRT-PCR）评估结肠癌组织中DUXAP8、微小RNA-378a-3p、FOXQ1的表达，并分析临床数据以确定DUXAP8表达与结肠癌患者预后之间的相关性。利用核/质RNA分级分离法分析DUXAP8的亚细胞分布。进行双荧光素酶和RNA免疫沉淀试验以证实DUXAP8/FOXQ1与微小RNA-378a-3p的结合。细胞转染后，采用qRT-PCR评估DUXAP8/微小RNA-378a-3p/FOXQ1的调节关系。采用细胞计数试剂盒-8、MTT、划痕愈合和Transwell试验评估DUXAP8/微小RNA-378a-3p/FOXQ1表达对结肠癌细胞功能的影响。

结果

结果显示，结肠癌组织中DUXAP8和FOXQ1的表达上调，而微小RNA-378a-3p的表达下调。DUXAP8表达增加与淋巴结转移和TNM分期呈正相关。双荧光素酶和RNA免疫沉淀试验表明，DUXAP8是微小RNA-378a-3p的海绵，靶向微小RNA-378a-3p调节FOXQ1的能力。此外，功能实验结果显示，过表达DUXAP8促进结肠癌细胞的生长和迁移能力。DUXAP8还逆转了微小RNA-378a-3p的抑癌作用。然而，沉默FOXQ1可逆转高DUXAP8表达的促癌作用。