Zhang Ming, Gao Chang'e, Yang Yi, Li Gaofeng, Dong Jian, Ai Yiqin, Ma Qianli, Li Wenhui
Department of Radiation Oncology, The Third Affiliated Hospital of Kunming Medical University, Tumor Hospital of Yunnan Province, Kunming, China.
Department of Medical Oncology, The First Affiliated Hospital of Kunming Medical University, Kunming, China.
Cell Physiol Biochem. 2017;42(1):211-221. doi: 10.1159/000477314. Epub 2017 May 25.
BACKGROUND/AIMS: This study aimed to investigate the potential roles of miR-424 expression in non-small cell lung cancer (NSCLC) metastasis and growth and its underlying mechanism.
The expression of miR-424 in two NSCLC cell lines (A549 and H1975) was altered by transfection with miR-424 mimic and inhibitor. Effects of miR-424 overexpression and suppression on cells migration, invasion and colony formation were analyzed. Target genes for miR-424 were predicted using bioinformatics method and then verified using luciferase assay. Effects of miR-424 expression on cell migration, invasion and proliferation were reanalyzed on the condition of TNFAIP1 was silenced. Moreover, TNFAIP1 silencing and miR-424 modified A549 cells were subcutaneous injected into node BALB/c mice to confirm the regulation of miR-424 on TNFAIP1 in regulating tumor growth.
Compared with the control, miR-424 overexpression significantly increased the migrated and invaded cells, as well as the proliferated colonies. TNFAIP1 was a predicted target gene for miR-424, and was negatively regulated by miR-424. TNFAIP1 silence significantly increased the migrated and invaded cells compared to that in control, while these increases were abolished by miR-424 suppression. Animal experiment further evidenced miR-424 affected tumor growth by regulating TNFAIP1.
These data demonstrate that miR-424 may be a contributor for NSCLC progression and metastasis through involving in cell migration, invasion and proliferation via inhibiting TNFAIP1. This study may provide theoretical basis for miR-424 in NSCLC target therapeutic treatment.
背景/目的:本研究旨在探讨miR-424表达在非小细胞肺癌(NSCLC)转移和生长中的潜在作用及其潜在机制。
通过转染miR-424模拟物和抑制剂改变两种NSCLC细胞系(A549和H1975)中miR-424的表达。分析miR-424过表达和抑制对细胞迁移、侵袭和集落形成的影响。使用生物信息学方法预测miR-424的靶基因,然后通过荧光素酶测定进行验证。在TNFAIP1沉默的条件下,重新分析miR-424表达对细胞迁移、侵袭和增殖的影响。此外,将TNFAIP1沉默和miR-424修饰的A549细胞皮下注射到BALB/c裸鼠体内,以确认miR-424对TNFAIP1在调节肿瘤生长中的调控作用。
与对照组相比,miR-424过表达显著增加了迁移和侵袭的细胞以及增殖的集落。TNFAIP1是miR-424的预测靶基因,并受到miR-424的负调控。与对照组相比,TNFAIP1沉默显著增加了迁移和侵袭的细胞,而这些增加被miR-424抑制所消除。动物实验进一步证明miR-424通过调节TNFAIP1影响肿瘤生长。
这些数据表明,miR-424可能通过抑制TNFAIP1参与细胞迁移、侵袭和增殖,从而促进NSCLC的进展和转移。本研究可能为miR-424在NSCLC靶向治疗中的应用提供理论依据。
