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Noninvasive evaluation of 18F-FDG/18F-FMISO-based Micro PET in monitoring hepatic metastasis of colorectal cancer

机译:基于18F-FDG / 18F-FMISO的微型PET在监测大肠癌肝转移中的无创评估

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摘要

This study aimed to explore the application of two radiotracers (18F-fluorodeoxyglucose (FDG) and 18F-fluoromisonidazole (FMISO)) in monitoring hepatic metastases of human colorectal cancer (CRC). Mouse models of CRC hepatic metastases were established by implantation of the human CRC cell lines LoVo and HT29 by intrasplenic injection. Wound healing and Transwell assays were performed to examine cell migration and invasion abilities. Radiotracer-based cellular uptake in vitro and micro-positron emission tomography imaging of liver metastases in vivo were performed. The incidence of liver metastases in LoVo-xenografted mice was significantly higher than that in HT29-xenografted ones. The SUVmax/mean values of 18F-FMISO, but not 18F-FDG, in LoVo xenografts were significantly greater than in HT29 xenografts. In vitro, LoVo cells exhibited stronger metastatic potential and higher radiotracer uptake than HT29 cells. Mechanistically, the expression of HIF-1α and GLUT-1 in LoVo cells and LoVo tumor tissues was remarkably higher than in HT29 cells and tissues. Linear regression analysis demonstrated correlations between cellular 18F-FDG/18F-FMISO uptake and HIF-1α/GLUT-1 expression in vitro, as well as between 18F-FMISO SUVmax and GLUT-1 expression in vivo. 18F-FMISO uptake may serve as a potential biomarker for the detection of liver metastases in CRC, whereas its clinical use warrants validation.
机译:本研究旨在探讨两种放射性示踪剂( 18 F-氟代脱氧葡萄糖(FDG)和 18 F-氟代咪唑(FMISO))在监测人类大肠癌肝转移中的应用( CRC)。通过脾内注射植入人CRC细胞系LoVo和HT29,建立CRC肝转移的小鼠模型。进行伤口愈合和Transwell测定以检查细胞迁移和侵袭能力。进行了基于放射性示踪剂的细胞体外吸收和体内肝转移的微正电子发射断层显像。 LoVo异种移植小鼠的肝转移发生率显着高于HT29异种移植小鼠。 LoVo异种移植物中 18 F-FMISO而不是 18 F-FDG的SUVmax /平均值明显高于HT29异种移植。在体外,LoVo细胞比HT29细胞表现出更强的转移潜能和更高的放射性示踪剂摄取。从机理上讲,LoVo细胞和LoVo肿瘤组织中HIF-1α和GLUT-1的表达明显高于HT29细胞和组织。线性回归分析显示了细胞 18 F-FDG / 18 F-FMISO摄取与体外HIF-1α/ GLUT-1表达之间以及之间的相关性18 F-FMISO SUVmax和GLUT-1在体内的表达。 18 F-FMISO摄取可能是检测CRC肝转移的潜在生物标志物,而其临床应用值得验证。

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