用 [18F]FLT 和 [18F]FDG PET 在荷人卵巢癌细胞移植瘤小鼠中早期检测对实验性化疗 Top216 的反应。
Early detection of response to experimental chemotherapeutic Top216 with [18F]FLT and [18F]FDG PET in human ovary cancer xenografts in mice.
机构信息
Cluster for Molecular Imaging, Faculty of Health Sciences, University of Copenhagen, Copenhagen, Denmark.
出版信息
PLoS One. 2010 Sep 24;5(9):e12965. doi: 10.1371/journal.pone.0012965.
BACKGROUND
3'-Deoxy-3'-[(18)F]fluorothymidine ((18)F-FLT) is a tracer used to assess cell proliferation in vivo. The aim of the study was to use (18)F-FLT positron emission tomography (PET) to study treatment responses to a new anti-cancer compound. To do so, we studied early anti-proliferative effects of the experimental chemotherapy Top216 non-invasively by PET.
METHODOLOGY/PRINCIPAL FINDINGS: In vivo uptake of (18)F-FLT in human ovary cancer xenografts in mice (A2780) was studied at various time points after Top216 treatment (50 mg/kg i.v. at 0 and 48 hours) was initiated. Baseline (18)F-FLT scans were made before either Top216 (n = 7-10) or vehicle (n = 5-7) was injected and repeated after 2 and 6 hours and 1 and 5 days of treatment. A parallel study was made with 2'-deoxy-2'-[(18)F]fluoro-D-glucose ((18)F-FDG) (n = 8). Tracer uptake was quantified using small animal PET/CT. Imaging results were validated by tumor volume changes and gene-expression of Ki67 and TK1. Top216 (50 mg/kg 0 and 48 hours) inhibited the growth of the A2780 tumor compared to the control group (P<0.001). (18)F-FLT uptake decreased significantly at 2 hours (-52%; P<0.001), 6 hours (-49%; P = 0.002) and Day 1 (-47%; P<0.001) after Top216 treatment. At Day 5 (18)F-FLT uptake was comparable to uptake in the control group. Uptake of (18)F-FLT was unchanged in the control group during the experiment. In the treatment group, uptake of (18)F-FDG was significantly decreased at 6 hours (-21%; P = 0.003), Day 1 (-29%; P<0.001) and Day 5 (-19%; P = 0.05) compared to baseline.
CONCLUSIONS/SIGNIFICANCE: One injection with Top216 initiated a fast and significant decrease in cell-proliferation assessable by (18)F-FLT after 2 hours. The early reductions in tumor cell proliferation preceded changes in tumor size. Our data indicate that (18)F-FLT PET is promising for the early non-invasive assessment of chemotherapy effects in both drug development and for tailoring therapy in patients.
背景
3'-脱氧-3'-[(18)F]氟胸苷((18)F-FLT)是一种用于评估体内细胞增殖的示踪剂。本研究的目的是使用(18)F-FLT 正电子发射断层扫描(PET)来研究新抗癌化合物的治疗反应。为此,我们通过 PET 研究了实验性化疗 Top216 对增殖的早期抗作用。
方法/主要发现:在开始给予 Top216(50mg/kg 静脉注射,0 和 48 小时)后,在不同时间点研究了人类卵巢癌异种移植(A2780)中(18)F-FLT 的体内摄取。在注射 Top216(n=7-10)或载体(n=5-7)之前进行基线(18)F-FLT 扫描,并在 2、6 小时和 1、5 天后重复扫描。还进行了平行的 2'-脱氧-2'-[(18)F]氟-D-葡萄糖((18)F-FDG)(n=8)研究。使用小动物 PET/CT 定量测量示踪剂摄取。通过肿瘤体积变化和 Ki67 和 TK1 的基因表达来验证成像结果。与对照组相比,Top216(50mg/kg 0 和 48 小时)抑制了 A2780 肿瘤的生长(P<0.001)。在 Top216 治疗后 2 小时(-52%;P<0.001)、6 小时(-49%;P=0.002)和第 1 天(-47%;P<0.001),(18)F-FLT 摄取显著降低。在第 5 天(18)F-FLT 摄取与对照组相似。对照组在实验过程中摄取(18)F-FLT 不变。在治疗组中,与基线相比,6 小时(-21%;P=0.003)、第 1 天(-29%;P<0.001)和第 5 天(-19%;P=0.05)的(18)F-FDG 摄取显著降低。
结论/意义:单次注射 Top216 可在 2 小时后快速且显著降低细胞增殖,通过(18)F-FLT 可评估。肿瘤细胞增殖的早期减少先于肿瘤大小的变化。我们的数据表明,(18)F-FLT PET 有望用于早期非侵入性评估药物开发中的化疗效果,并为患者的治疗提供指导。
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