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Noninvasive indirect imaging of vascular endothelial growth factor gene expression using bioluminescence imaging in living transgenic mice

机译:使用生物发光成像技术对活体转基因小鼠进行血管内皮生长因子基因表达的非侵入性间接成像

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Vascular endothelial growth factor (VEGF) plays a critical role in the early activation of stromal tissues during wound healing and tumor growth. We report the use of a two-step transcriptional amplification (TSTA) approach to augment the transcriptional activity of the relatively weak VEGF promoter (pVEGF) using firefly luciferase (fl) reporter gene and bioluminescence imaging (BLI). In cell culture, we demonstrate that TSTA-based fl gene expression can be significantly enhanced over the direct one-step system. Using a transgenic mouse model (pVEGF-TSTAfl), we demonstrate the induction of VEGF gene expression using a wound-healing model and a subcutaneous mammary tumor model. In skin-wounding experiments, pVEGF-induced fl expression in the wound lesion is detected on days 4 and 5 and peaks on days 15-22. Furthermore, the bioluminescence signal shows good correlation with the endogenous VEGF protein levels in the wound tissue (r(2) = 0.70). In the mammary tumor model, fl expression is detected on day 3, peaks at day 17, and declines thereafter. These results support the use of noninvasive BLI for the longitudinal monitoring of VEGF induction during wound healing and tumor progression, and this mouse model should find use in various applications in which it is important to noninvasively study VEGF gene expression.
机译:血管内皮生长因子(VEGF)在伤口愈合和肿瘤生长过程中在基质组织的早期活化中起关键作用。我们报告了使用萤火虫荧光素酶(fl)报告基因和生物发光成像(BLI)的两步转录扩增(TSTA)方法来增强相对较弱的VEGF启动子(pVEGF)的转录活性。在细胞培养中,我们证明了基于TSTA的fl基因表达可以比直接一步系统显着增强。使用转基因小鼠模型(pVEGF-TSTAf1),我们证明了使用伤口愈合模型和皮下乳腺肿瘤模型诱导VEGF基因表达。在皮肤创伤实验中,在伤口的第4天和第5天检测到pVEGF诱导的fl表达,在第15-22天达到峰值。此外,生物发光信号与伤口组织中的内源性VEGF蛋白水平显示出良好的相关性(r(2)= 0.70)。在乳腺肿瘤模型中,在第3天检测到fl表达,在第17天达到峰值,此后下降。这些结果支持在伤口愈合和肿瘤进展过程中使用非侵入性BLI纵向监测VEGF的诱导作用,并且该小鼠模型应该用于对非侵入性研究VEGF基因表达很重要的各种应用中。

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