(18)F-FDG与(18)F-FMISO联合应用于计划接受放疗的不可切除非小细胞肺癌患者:一项动态PET/CT研究
Combined use of (18)F-FDG and (18)F-FMISO in unresectable non-small cell lung cancer patients planned for radiotherapy: a dynamic PET/CT study.
作者信息
Sachpekidis Christos, Thieke Christian, Askoxylakis Vasileios, Nicolay Nils H, Huber Peter E, Thomas Michael, Dimitrakopoulou Georgia, Debus Juergen, Haberkorn Uwe, Dimitrakopoulou-Strauss Antonia
机构信息
Clinical Cooperation Unit Nuclear Medicine, German Cancer Research Center Heidelberg, Germany.
Clinical Cooperation Unit Radiotherapy, German Cancer Research Center Heidelberg, Germany ; Department of Radiation Oncology, University Clinic Heidelberg Germany.
出版信息
Am J Nucl Med Mol Imaging. 2015 Jan 15;5(2):127-42. eCollection 2015.
Aim of this study was to evaluate and compare, by means of dynamic and static PET/CT, the distribution patterns and pharmacokinetics of fluorine-18 fluorodeoxyglucose ((18)F-FDG) and of fluorine-18-fluoromisonidazole ((18)F-FMISO) in non-small cell lung cancer (NSCLC) patients scheduled for intensity modulated radiation therapy (IMRT). Thirteen patients suffering from inoperable stage III NSCLC underwent PET/CTs with (18)F-FDG and (18)F-FMISO for tumor metabolism and hypoxia assessment accordingly. Evaluation of PET/CT studies was based on visual analysis, semi-quantitative (SUV) calculations and absolute quantitative estimations, after application of a two-tissue compartment model and a non-compartmental approach. (18)F-FDG PET/CT revealed all thirteen primary lung tumors as sites of increased (18)F-FDG uptake. Six patients demonstrated also in total 43 (18)F-FDG avid metastases; these patients were excluded from radiotherapy. (18)F-MISO PET/CT demonstrated 12/13 primary lung tumors with faint tracer uptake. Only one tumor was clearly (18)F-FMISO avid, (SUVaverage = 3.4, SUVmax = 5.0). Mean values for (18)F-FDG, as derived from dPET/CT data, were SUVaverage = 8.9, SUVmax = 15.1, K1 = 0.23, k2 = 0.53, k3 = 0.17, k4 = 0.02, influx = 0.05 and fractal dimension (FD) = 1.25 for the primary tumors. The respective values for (18)F-FMISO were SUVaverage = 1.4, SUVmax = 2.2, K1 = 0.26, k2 = 0.56, k3 = 0.06, k4 = 0.06, influx = 0.02 and FD = 1.14. No statistically significant correlation was observed between the two tracers. (18)F-FDG PET/CT changed therapy management in six patients, by excluding them from planned IMRT. (18)F-FMISO PET/CT revealed absence of significant tracer uptake in the majority of the (18)F-FDG avid NSCLCs. Lack of correlation between the two tracers' kinetics indicates that they reflect different molecular mechanisms and implies the discordance between increased glycolysis and hypoxia in the malignancy.
本研究的目的是通过动态和静态PET/CT评估并比较氟-18氟脱氧葡萄糖((18)F-FDG)和氟-18氟米索硝唑((18)F-FMISO)在计划接受调强放射治疗(IMRT)的非小细胞肺癌(NSCLC)患者中的分布模式和药代动力学。13例患有无法手术的III期NSCLC患者分别接受了(18)F-FDG和(18)F-FMISO的PET/CT检查,以评估肿瘤代谢和缺氧情况。在应用双组织室模型和非房室方法后,基于视觉分析、半定量(SUV)计算和绝对定量估计对PET/CT研究进行评估。(18)F-FDG PET/CT显示所有13个原发性肺肿瘤均为(18)F-FDG摄取增加的部位。6例患者共发现43个(18)F-FDG摄取阳性的转移灶;这些患者被排除在放射治疗之外。(18)F-MISO PET/CT显示13个原发性肺肿瘤中有12个示踪剂摄取微弱。只有一个肿瘤明显(18)F-FMISO摄取阳性(SUV平均值 = 3.4,SUV最大值 = 5.0)。从动态PET/CT数据得出的(18)F-FDG的平均值为:原发性肿瘤的SUV平均值 = 8.9,SUV最大值 = 15.1,K1 = 0.23,k2 = 0.53,k3 = 0.17,k4 = 0.02,流入率 = 0.05,分形维数(FD) = 1.25。(18)F-FMISO的相应值为:SUV平均值 = 1.4,SUV最大值 = 2.2,K1 = 0.26,k2 = 0.56,k3 = 0.06,k4 = 0.06,流入率 = 0.02,FD = 1.14。两种示踪剂之间未观察到统计学上的显著相关性。(18)F-FDG PET/CT改变了6例患者的治疗管理,将他们排除在计划的IMRT之外。(18)F-FMISO PET/CT显示大多数(18)F-FDG摄取阳性的NSCLC中示踪剂摄取无显著增加。两种示踪剂动力学之间缺乏相关性表明它们反映了不同的分子机制,意味着恶性肿瘤中糖酵解增加与缺氧之间存在不一致。
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