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Differential Expression of miRNAs in Hypoxia (“HypoxamiRs”) in Three Canine High-Grade Glioma Cell Lines

机译:三种犬高级胶质瘤细胞缺氧中miRNA在缺氧(“缺氧”)的差异表达

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Dogs with spontaneous high-grade gliomas increasingly are being proposed as useful large animal pre-clinical models for the human disease. Hypoxia is a critical microenvironmental condition that is common in both canine and human high-grade gliomas and drives increased angiogenesis, chemo- and radioresistance, and acquisition of a stem-like phenotype. Some of this effect is mediated by the hypoxia-induced expression of microRNAs, small (~22 nucleotides long), non-coding RNAs that can modulate gene expression through interference with mRNA translation. Using an in vitro model with three canine high-grade glioma cell lines (J3T, SDT3G, and G06A) exposed to 72 hours of 1.5% oxygen versus standard 20% oxygen, we examined the global “hypoxamiR” profile using small RNA-Seq and performed pathway analysis for targeted genes using both Panther and NetworkAnalyst. Important pathways include many that are well-established as being important in glioma biology, general cancer biology, hypoxia, angiogenesis, immunology, and stem-ness, among others. This work provides the first examination of the effect of hypoxia on miRNA expression in the context of canine glioma, and highlights important similarities with the human disease.
机译:具有自发性高级胶质瘤的狗越来越多地被提出为人类疾病的有用的大型动物前临床模型。缺氧是一种关键的微环境条件,在犬和人的高级胶质瘤中常见,并且驱动增加的血管生成,化学和放射线,以及获取干燥的表型。一些这种效果是由缺氧诱导的微小RNA表达介导的微小(〜22个核苷酸长),无编码RNA,其可以通过干扰MRNA翻译来调节基因表达。使用具有三个犬高级胶质瘤细胞系(J3T,SDT3G和G06A)的体外模型暴露于72小时的1.5%氧与标准20%氧气,我们使用小型RNA-SEQ检查了全球“鼠尾草”型谱使用Panther和NetworlAnalyst进行靶向基因进行的途径分析。重要途径包括许多良好的途径,如在胶质瘤生物学,一般癌症生物学,缺氧,血管生成,免疫学和词干等中的重要性。这项工作提供了第一次检查缺氧对犬类胶质瘤背景下miRNA表达的影响,并突出了与人类疾病的重要相似之处。

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