Correlation of 18F-Fluorodeoxyglucose Glucose Uptake by Liver Cancer and Transcriptional Regulation of the Warburg Effects in ATT-MYC Mouse Model of Liver Cancer

M. Elalfy, J. Borlak
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引用次数: 1

Abstract

Background It was previously reported that diethylnitrosamine (DEN) enhanced liver cancer progression in ATT-MYC mouse model of liver cancer. Radiogenomics is a new tool in advanced science technology that gives information on tumor biology, non-tumor surrounding tissue, the degree of tumor size and presence of necrosis of cells especially with joined micro computed tomography – positron emission tomographys (CT/PETs). Aim To evaluate the correlation of gene expression and non-invasive microPET information of the liver tumors at different points of the stage of growth. Methods Exon array expression of the liver of ATT-MYC mice treated with DEN or butylated hydroxytoluene (BHT) compared to control non-transgenic mice were analyzed by array track and the current data were also compared to microarray expression of liver tumor of ATT-MYC mice. Results The expression of genes responsible for glucose transport such as glut1, 3, 4, hk1, slc1a5, slc1a1, slc1a4, slc1a2, gp6c and gpc-1-3-4 were up-regulated significantly in DEN-treated transgenic mice immediately after end of treatment (p≤0.05), while glut2 (fold change 0.9503, p-value 0.4385) and hk2 (fold change 3.0589, p-value 0.0565) genes were increased not significantly immediately after end of treatment. Additionally, at 4.5-months of observation after the end of treatment slc1a5, slc38a2, glut1, glut4 and gpc3-4 genes had a significant fold change in liver tumor tissue in DEN treated mice when compared to BHT or control transgenic or non-transgenic one. While hk1, 2, slc5a1, slc1a4, glut2, glut3, g6pc and gpc-1 genes were increased non-significantly in the liver of treated mice when compared to control group at 4.5-months of observation after the end of treatment. Notably, c-myc, hif-1 and aldoa glycolytic genes were expressed significantly both time points of 4 and 8.5-months while ldhb, hk-2 and PKM2 were increased non-significantly in DEN treatment when compared to BHT/control non-transgenic animals. Conclusion There is a definitive correlation between genes responsible for glucose transport and 18F-Fluorodeoxyglucose (FDG) uptake in the early and advanced degree of liver carcinogenesis. This study of glucose pathway in Hepatocellular carcinoma (HCC) at different stages of early and advanced one is the potential for therapeutic anticancer therapy.
肝癌18f -氟脱氧葡萄糖摄取与at - myc肝癌小鼠模型Warburg效应转录调控的相关性
背景先前有报道称,在at - myc肝癌小鼠模型中,二乙基亚硝胺(DEN)可促进肝癌的进展。放射基因组学是一种先进科学技术的新工具,它可以提供肿瘤生物学、非肿瘤周围组织、肿瘤大小程度和细胞坏死的信息,特别是与微型计算机断层扫描-正电子发射断层扫描(CT/ pet)结合。目的探讨肝肿瘤不同生长阶段基因表达与无创pet信息的相关性。方法采用阵列跟踪法分析经DEN或丁基羟基甲苯(BHT)处理的at - myc小鼠肝脏外显子阵列表达与对照非转基因小鼠的差异,并将当前数据与at - myc小鼠肝脏肿瘤微阵列表达进行比较。结果经dena处理的转基因小鼠葡萄糖转运相关基因glut1、3、4、hk1、slc1a5、slc1a1、slc1a4、slc1a2、gp6c和gpc-1-3-4的表达量在处理结束后立即显著上调(p≤0.05),glut2 (fold change 0.9503, p值0.4385)和hk2 (fold change 3.0589, p值0.0565)基因表达量在处理结束后立即不显著升高。此外,在治疗结束后4.5个月的观察中,与BHT或对照转基因或非转基因小鼠相比,DEN治疗小鼠肝肿瘤组织中slc1a5、slc38a2、glut1、glut4和gpc3-4基因发生了显著的翻倍变化。治疗结束后4.5个月观察时,治疗组小鼠肝脏中hk1、2、slc5a1、slc1a4、glut2、glut3、g6pc、gpc-1基因与对照组相比无显著性升高。值得注意的是,在4个月和8.5个月的时间点上,与BHT/对照非转基因动物相比,DEN治疗组c-myc、hif-1和醛糖酵解基因均有显著表达,而ldhb、hk-2和PKM2均无显著升高。结论在肝癌发生的早期和晚期,葡萄糖转运基因与18f -氟脱氧葡萄糖(FDG)摄取有明确的相关性。本研究对早期和晚期不同阶段肝细胞癌(HCC)中葡萄糖通路的研究为治疗性抗癌治疗提供了可能。
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