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BMC Molecular Biology (1)
PLoS ONE (1)
Authors
Peng, Xiaozhong (2)
Tan, Xiaochao (2)
Yin, Bin (2)
Chao, Tengfei (1)
Li, Jun (1)
Pan, Hui (1)
Qiang, Boqin (1)
Wang, Shan (1)
Yang, Bin (1)
Yuan, Jiangang (1)
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Year of Publication
2012 (2)
Document Types
research-article (2)
1.  The CREB-miR-9 Negative Feedback Minicircuitry Coordinates the Migration and Proliferation of Glioma Cells 
Tan, Xiaochao | Wang, Shan | Yang, Bin | Zhu, Liyuan | Yin, Bin | Chao, Tengfei | Zhao, Jizong | Yuan, Jiangang | Qiang, Boqin | Peng, Xiaozhong | Li, Jun
PLoS ONE  2012;7(11):e49570.
Migration-proliferation dichotomy is a common mechanism in gliomagenesis; however, an understanding of the exact molecular mechanism of this “go or grow” phenomenon remains largely incomplete. In the present study, we first found that microRNA-9 (miR-9) is highly expressed in glioma cells. MiR-9 inhibited the proliferation and promoted the migration of glioma cells by directly targeting cyclic AMP response element-binding protein (CREB) and neurofibromin 1 (NF1), respectively. Our data also suggested a migration-inhibitory role for CREB through directly regulating the transcription of NF1. Furthermore, we found that the transcription of miR-9-1 is under CREB's control, forming a negative feedback minicircuitry. Taken together, miR-9 inhibits proliferation but promotes migration, whereas CREB plays a pro-proliferative and anti-migratory role, suggesting that the CREB-miR-9 negative feedback minicircuitry plays a critical role in the determination of “go or grow” in glioma cells.
doi:10.1371/journal.pone.0049570
PMCID: PMC3502497  PMID: 23185366
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2.  Clock-controlled mir-142-3p can target its activator, Bmal1 
Tan, Xiaochao | Zhang, Peng | Zhou, Lan | Yin, Bin | Pan, Hui | Peng, Xiaozhong
BMC Molecular Biology  2012;13:27.
Background
microRNAs (miRNAs) are shown to be involved in the regulation of circadian clock. However, it remains largely unknown whether miRNAs can regulate the core clock genes (Clock and Bmal1).
Results
In this study, we found that mir-142-3p directly targeted the 3’UTR of human BMAL1 and mouse Bmal1. The over-expression (in 293ET and NIH3T3 cells) and knockdown (in U87MG cells) of mir-142-3p reduced and up-regulated the Bmal1/BMAL1 mRNA and protein levels, respectively. Moreover, the expression level of mir-142-3p oscillated in serum-shocked NIH3T3 cells and the results of ChIP and luciferase reporter assays suggested that the expression of mir-142-3p was directly controlled by CLOCK/BMAL1 heterodimers in NIH3T3 cells.
Conclusions
Our study demonstrates that mir-142-3p can directly target the 3’UTR of Bmal1. In addition, the expression of mir-142-3p is controlled by CLOCK/BMAL1 heterodimers, suggesting a potential negative feedback loop consisting of the miRNAs and the core clock genes. These findings open new perspective for studying the molecular mechanism of circadian clock.
doi:10.1186/1471-2199-13-27
PMCID: PMC3482555  PMID: 22958478
mir-142-3p; Bmal1; Circadian clock
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