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微小 RNA-130a 抑制水通道蛋白 4 M1 启动子的转录活性。

MicroRNA-130a represses transcriptional activity of aquaporin 4 M1 promoter.

机构信息

Department of Biochemistry and Neuroscience Research Centre, Yong Loo Lin School of Medicine, National University of Singapore, 8 Medical Drive, Singapore 117597, Singapore.

出版信息

J Biol Chem. 2012 Apr 6;287(15):12006-15. doi: 10.1074/jbc.M111.280701. Epub 2012 Feb 13.

Abstract

Aquaporins (AQPs) are transmembrane water channels ubiquitously expressed in mammalian tissues. They play prominent roles in maintaining cellular fluid balance. Although expression of AQP1, -3, -4, -5, -8, -9, and -11 has been reported in the central nervous system, it is AQP4 that is predominately expressed. Its importance in fluid regulation in cerebral edema conditions has been highlighted in several studies, and we have also shown that translational regulation of AQP4 by miR-320a could prove to be useful in infarct volume reduction in middle cerebral artery occluded rat brain. There is evidence for the existence of two AQP4 transcripts (M1 and M23) in the brain arising from two alternative promoters. Because the AQP4 M1 isoform exhibits greater water permeability, in this study, we explored the possibility of microRNA-based transcriptional regulation of the AQP4 M1 promoter. Using RegRNA software, we identified 34 microRNAs predicted to target the AQP4 M1 promoter region. MicroRNA profiling, quantitative stem-loop PCR, and luciferase reporter assays revealed that miR-130a, -152, -668, -939, and -1280, which were highly expressed in astrocytes, could regulate the promoter activity. Of these, miR-130a was identified as a strong transcriptional repressor of the AQP4 M1 isoform. In vivo studies revealed that LNA(TM) anti-miR-130a could up-regulate the AQP4 M1 transcript and its protein to bring about a reduction in cerebral infarct and promote recovery.

摘要

水通道蛋白(AQP)是广泛表达于哺乳动物组织的跨膜水分子通道。它们在维持细胞液平衡方面发挥着重要作用。虽然已有研究报道 AQP1、-3、-4、-5、-8、-9 和 -11 在中枢神经系统中表达,但主要表达的是 AQP4。在脑水肿情况下,AQP4 在液体调节中的重要性已在多项研究中得到强调,我们还表明,miR-320a 对 AQP4 的翻译调控可能有助于减少大脑中动脉闭塞大鼠脑梗死体积。有证据表明,脑内存在两种 AQP4 转录本(M1 和 M23),它们来源于两个不同的启动子。由于 AQP4 M1 异构体表现出更高的水通透性,因此在本研究中,我们探讨了基于 microRNA 的 AQP4 M1 启动子转录调控的可能性。使用 RegRNA 软件,我们鉴定出 34 个 microRNA 可能靶向 AQP4 M1 启动子区域。microRNA 谱分析、定量茎环 PCR 和荧光素酶报告基因检测显示,在星形胶质细胞中高表达的 miR-130a、-152、-668、-939 和 -1280 可以调节启动子活性。其中,miR-130a 被鉴定为 AQP4 M1 异构体的强转录抑制剂。体内研究表明,LNA(TM) 抗 miR-130a 可以上调 AQP4 M1 转录本及其蛋白,从而减少脑梗死并促进恢复。

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