生物
KLF2
癌变
基因沉默
细胞生长
下调和上调
癌症研究
细胞凋亡
细胞生物学
分子生物学
癌症
基因
遗传学
作者
T-p Xu,Liu Xx,Ran Xia,Lei Yin,Rong Kong,W-m Chen,M-d Huang,Y-q Shu
出处
期刊:Oncogene
[Springer Nature]
日期:2015-03-02
卷期号:34 (45): 5648-5661
被引量:257
摘要
The long noncoding RNA TINCR shows aberrant expression in human squamous carcinomas. However, its expression and function in gastric cancer remain unclear. We report that TINCR is strongly upregulated in human gastric carcinoma (GC), where it was found to contribute to oncogenesis and cancer progression. We also revealed that TINCR overexpression is induced by nuclear transcription factor SP1. Silencing TINCR expression inhibited cell proliferation, colony formation, tumorigenicity and apoptosis promotion, whereas TINCR overexpression promoted cell growth, as documented in the SGC7901 and BGC823 cell lines. Mechanistic analyses indicated that TINCR could bind to STAU1 (staufen1) protein, and influence KLF2 mRNA stability and expression, then KLF2 regulated cyclin-dependent kinase genes CDKN1A/P21 and CDKN2B/P15 transcription and expression, thereby affecting the proliferation and apoptosis of GC cells. Together, our findings suggest that TINCR contributes to the oncogenic potential of GC and may constitute a potential therapeutic target in this disease.
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