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Cellular uptake of PET tracers of glucose metabolism and hypoxia and their linkage.

机译:葡萄糖代谢和缺氧的PET示踪剂的细胞摄取及其联系。

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PURPOSE: Tumour hypoxia and elevated glycolysis (Warburg effect) predict poor prognosis. Each parameter is assessable separately with positron emission tomography, but they are linked through anaerobic glycolysis (Pasteur effect). Here, we compare the oxygenation-dependent retention of fluoroazomycin arabinoside ([(18)F]FAZA), a promising but not well-characterised hypoxia-specific tracer, and fluorodeoxyglucose ([(18)F]FDG) in four carcinoma cell lines. METHODS: Cells seeded on coverslips were positioned in modified Petri dishes that allow physically separated cells to share the same tracer-containing medium pool. Following oxic, hypoxic or anoxic tracer incubation, coverslips were analysed for radioactivity ([(18)F]FDG + [(18)F]FAZA) or re-incubated in tracer-free oxygenated medium and then measured ([(18)F]FAZA). Next, we tested the reliability of [(18)F]FDG as a relative measure of glucose metabolic rate. Finally, from two cell lines, xenografts were established in mice, and the tracer distributionbetween hypoxic and well-oxygenated areas were deduced from tissue sections. RESULTS: Three hours of anoxia strongly stimulated [(18)F]FAZA retention with anoxic-to-oxic uptake ratios typically above 30. Three out of four cell lines displayed similar selectivity of [(18)F]FDG versus glucose, but oxic uptake and anoxic-to-oxic uptake ratio of [(18)F]FDG varied considerably. Although less pronounced, [(18)F]FAZA also showed superior in vivo hypoxia specificity compared with [(18)F]FDG. CONCLUSIONS: [(18)F]FAZA displays excellent in vitro characteristics for hypoxia imaging including modest cell-to-cell line variability and no binding in oxic cells. In contrast, the usability of [(18)F]FDG as a surrogate marker for hypoxia is questionable due to large variations in baseline (oxic) glucose metabolism and magnitudes of the Pasteur effects.
机译:目的:肿瘤缺氧和糖酵解升高(Warburg效应)预后不良。每个参数都可以用正电子发射断层显像法单独评估,但是它们通过厌氧糖酵解(Pasteur效应)联系在一起。在这里,我们比较了氟阿霉素阿糖苷([(18)F] FAZA),一种有前途但不是很好表征的缺氧特异性示踪剂和氟脱氧葡萄糖([(18)F] FDG)在四种癌细胞系中的氧合依赖性保留。方法:将盖玻片上接种的细胞置于改良的陪替氏培养皿中,使物理分离的细胞共享相同的含示踪剂的培养基库。在有氧,低氧或缺氧示踪剂孵育后,分析盖玻片的放射性([(18)F] FDG + [(18)F] FAZA)或在无示踪剂的含氧培养基中重新孵育,然后进行测量([[18] F ] FAZA)。接下来,我们测试了[(18)F] FDG作为葡萄糖代谢率的相对量度的可靠性。最后,从两种细胞系中,在小鼠中建立异种移植物,并从组织切片中推断出在低氧和氧合良好区域之间的示踪剂分布。结果:3个小时的缺氧强烈刺激[(18)F] FAZA的保留​​,缺氧与氧的摄取比率通常高于30。四分之三的细胞系对[(18)F] FDG与葡萄糖的选择性相似,但有氧[(18)F] FDG的摄取量和缺氧/有氧摄取率差异很大。尽管不太明显,但[(18)F] FAZA与[(18)F] FDG相比,体内缺氧特异性更高。结论:[(18)F] FAZA缺氧成像显示出色的体外特征,包括适度的细胞间变化,在含氧细胞中无结合。相比之下,[(18)F] FDG作为缺氧的替代标志物的可用性令人质疑,这是因为基线(有氧)葡萄糖代谢和巴斯德效应的幅度存在较大差异。

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