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miR-192, miR-194, miR-215, miR-200c and miR-141 are downregulated and their common target ACVR2B is strongly expressed inn renal childhood neoplasms

机译:miR-192,miR-194,miR-215,miR-200c和miR-141被下调,并且它们的共同靶标ACVR2B在儿童肾小瘤中强烈表达

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Micro RNAs (miRNAs) play an important role during renal development and show a tissue-specific enrichment in the kidney. Nephroblastomas, embryonal renal neoplasms of childhood, are considered to develop from nephrogenic rests (NRs) and resemble morphologically and genetically developing kidney. We therefore investigated the role of kidney-enriched miRNAs in the pathogenesis of nephroblastomas. miR-192, miR-215 and miR-194 had a significantly lower expression in nephroblastomas regardless of the subtype compared with mature kidney measured by quantitative real-time–PCR. miR-141 and miR-200c showed a significantly lower expression in blastema-type and mixed-type tumors. In comparison with NRs, a significantly lower expression of miR-192, miR-194 and miR-215 was identified in blastema-type, mixed-type and stroma-type nephroblastomas and of miR-141 and miR-200c in blastema-type tumors. Kidney parenchyma had a significantly higher expression of miR-192, miR-194, miR-215 and miR-200c compared with NRs. In this study, the activin receptor type 2B (ACVR2B), a member of the transforming growth factor (TGF)-β pathway, was identified as single common target gene for miR-192, miR-215, miR-194, miR-141 and miR-200c in silico for the first time. The interaction between all five miRNAs and ACVR2B was also verified by an in vitro assay. Additionally, a distinct protein expression of ACVR2B was detected in 53 of 55 nephroblastomas paralleled by an upregulation of ACVR2B messenger RNA demonstrated in 25 nephroblastomas of all subtypes. A differential regulation of ACVR2B by miRNAs in NRs and nephroblastomas appears to be an important step in the pathogenesis of nephroblastomas implicating for the first time the TGF-β pathway in this process.
机译:微小RNA(miRNA)在肾脏发育过程中起重要作用,并在肾脏中表现出组织特异性富集。肾母细胞瘤,儿童期的胚胎肾脏肿瘤,被认为是从肾原性休克(NRs)发育而来,在形态和基因上都与肾脏相似。因此,我们研究了肾脏富集的miRNA在肾母细胞瘤的发病机理中的作用。与定量实时荧光定量PCR检测的成熟肾脏相比,无论亚型是什么,在肾母细胞瘤中miR-192,miR-215和miR-194的表达均显着降低。 miR-141和miR-200c在胚细胞型和混合型肿瘤中表达明显降低。与NRs相比,在母细胞样,混合型和基质型肾母细胞瘤中发现了miR-192,miR-194和miR-215的低表达,在母细胞瘤型肿瘤中发现了miR-141和miR-200c的表达。 。与NR相比,肾实质中miR-192,miR-194,miR-215和miR-200c的表达明显更高。在这项研究中,激活素2B型(ACVR2B)是转化生长因子(TGF)-β途径的成员,被确定为miR-192,miR-215,miR-194,miR-141的单个共同靶标基因和miR-200c首次在计算机上发布。所有五个miRNA与ACVR2B之间的相互作用也通过体外测定法进行了验证。另外,在55个肾母细胞瘤中的53个中检测到ACVR2B的独特蛋白表达,同时在所有亚型的25个肾母细胞瘤中证实了ACVR2B信使RNA的上调。 NRs和肾母细胞瘤中miRNA对ACVR2B的差异调节似乎是肾母细胞瘤发病机理中重要的一步,在此过程中首次涉及TGF-β途径。

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    《Carcinogenesis》 |2012年第5期|p.1014-1021|共8页
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  • 入库时间 2022-08-18 01:13:12

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