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Identification of microRNAs during rat liver regeneration after partial hepatectomy and modulation by ursodeoxycholic acid

机译:大鼠肝部分切除和熊去氧胆酸调节后的肝再生过程中的微小RNA的鉴定

摘要

New gene regulation study tools such as microRNA (miRNA or miR) analysis may provide unique insights into the remarkable ability of the liver to regenerate. In addition, we have previously shown that ursodeoxycholic acid (UDCA) modulates mRNA levels during liver regeneration. Bile acids are also homeotrophic sensors of functional hepatic capacity. The present study was designed to determine whether miRNAs are modulated in rats following 70% partial hepatectomy (PH) and elucidate the role of UDCA in regulating miRNA expression during liver regeneration (LR). Total RNA was isolated from livers harvested at 3–72 h following 70% PH or sham operations, from both 0.4% (wt/wt) UDCA and control diet-fed animals. By using a custom microarray platform we found that several miRNAs are significantly altered after PH by >1.5-fold, including some previously described as modulators of cell proliferation, differentiation, and death. In particular, expression of miR-21 was increased after PH. Functional modulation of miR-21 in primary rat hepatocytes increased cell proliferation and viability. Importantly, UDCA was a strong inducer of miR-21 both during LR and in cultured HepG2 cells. In fact, UDCA feeding appeared to induce a sustained increase of proliferative miRNAs observed at early time points after PH. In conclusion, miRNAs, in particular miR-21, may play a significant role in modulating proliferation and cell cycle progression genes after PH. miR-21 is additionally induced by UDCA in both regenerating rat liver and in vitro, which may represent a new mechanism behind UDCA biological functions.
机译:诸如microRNA(miRNA或miR)分析之类的新基因调控研究工具可以提供有关肝脏再生能力的独特见解。此外,我们以前已经证明,熊去氧胆酸(UDCA)在肝脏再生过程中调节mRNA水平。胆汁酸也是功能肝功能的同养型传感器。本研究旨在确定70%部分肝切除术(PH)后大鼠中是否调节了miRNA,并阐明了UDCA在肝脏再生(LR)过程中调控miRNA表达的作用。从pH值为70%或假手术的3–72 h采集的肝脏中分离总RNA,分别来自0.4%(wt / wt)UDCA和对照饮食喂养的动物。通过使用定制的微阵列平台,我们发现PH值后,若干miRNA的变化显着> 1.5倍,包括一些先前描述为细胞增殖,分化和死亡的调节剂。特别地,PH后miR-21的表达增加。原代大鼠肝细胞中miR-21的功能性调节可增加细胞增殖和活力。重要的是,无论是在LR还是在培养的HepG2细胞中,UDCA都是miR-21的强力诱导剂。实际上,在PH发生后的早期观察到,UDCA喂养似乎诱导了增殖性miRNA的持续增加。总之,miRNA,特别是miR-21,在PH后可能在调节增殖和细胞周期进程基因中起重要作用。 UDCA还可以在再生大鼠肝脏和体外诱导miR-21,这可能是UDCA生物学功能背后的新机制。

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