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Integrated analysis of microRNA and mRNA expression profiles in splenomegaly induced by non-cirrhotic portal hypertension in rats

机译:非肝硬化门脉高压大鼠脾肿大中微小RNA和mRNA表达谱的综合分析

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The spleen plays an important role in the immune and hematopoietic systems. Splenomegaly is a frequent consequence of portal hypertension, but the underlying molecular and cellular mechanisms remain to be fully elucidated. In this study, we have performed a whole-genome microarray analysis combined with histological examination in enlarged spleens isolated from rats with partial portal vein ligation (PPVL) surgery to provide comprehensive profiles of microRNAs and their target mRNAs with a focus on their potential biological functions. A total of 964 mRNAs and 30 microRNAs showed significant differential expression in the spleens of PPVL rats compared to rats undergoing a sham procedure. Twenty-two down-regulated microRNAs were associated with significantly increased genes highly involved in fibrogenic activity and cell proliferation/migration (e.g., Ctgf, Serpine1, Col1a1). Consistently, histological analyses demonstrated increased splenic fibrosis and cell proliferation in the spleens of PPVL rats. Eight up-regulated microRNAs were associated with suppression of genes that are related to interferon-mediated antiviral activity in innate immune responses (e.g., Irf7, Dhx58). In conclusion, we determined a specific microRNA-mRNA network potentially implicated in the tissue fibrosis and cell proliferation in portal hypertension-induced splenomegaly. Our findings provide new insight into the mechanisms for regulation of spleen structure and function.
机译:脾脏在免疫和造血系统中起重要作用。脾肿大是门静脉高压症的常见后果,但其潜在的分子和细胞机制尚待充分阐明。在这项研究中,我们进行了全基因组微阵列分析并结合组织学检查,对部分门静脉结扎术(PPVL)的大鼠分离出的脾脏进行了放大,以提供microRNA及其靶标mRNA的全面概况,重点是其潜在的生物学功能。与进行假手术的大鼠相比,PPVL大鼠的脾脏中总共有964个mRNA和30个microRNA表现出明显的差异表达。 22个下调的microRNA与显着增加的基因高度相关,这些基因高度参与了纤维形成活性和细胞增殖/迁移(例如Ctgf,Serpine1,Col1a1)。一致地,组织学分析显示PPVL大鼠脾脏中脾纤维化和细胞增殖增加。八个上调的microRNA与固有免疫反应中干扰素介导的抗病毒活性相关基因的抑制有关(例如Irf7,Dhx58)。总之,我们确定了可能与门脉高压诱发的脾肿大中组织纤维化和细胞增殖有关的特定microRNA-mRNA网络。我们的发现为调节脾脏结构和功能的机制提供了新的见识。

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