Department of Radiology and Nuclear Medicine, VU University Medical Center, PO Box 7057, 1007 MB, Amsterdam, Netherlands.
European Organisation for Research and Treatment for Cancer (EORTC), Headquarters, Brussels, Belgium.
Eur J Nucl Med Mol Imaging. 2018 Jun;45(6):951-961. doi: 10.1007/s00259-017-3923-x. Epub 2018 Jan 23.
3'-deoxy-3'-[F]fluorothymidine (F-FLT) positron emission tomography (PET) provides a non-invasive method to assess cellular proliferation and response to antitumor therapy. Quantitative F-FLT uptake metrics are being used for evaluation of proliferative response in investigational setting, however multi-center repeatability needs to be established. The aim of this study was to determine the repeatability of F-FLT tumor uptake metrics by re-analyzing individual patient data from previously published reports using the same tumor segmentation method and repeatability metrics across cohorts.
A systematic search in PubMed, EMBASE.com and the Cochrane Library from inception-October 2016 yielded five F-FLT repeatability cohorts in solid tumors. F-FLT avid lesions were delineated using a 50% isocontour adapted for local background on test and retest scans. SUV, SUV, SUV, proliferative volume and total lesion uptake (TLU) were calculated. Repeatability was assessed using the repeatability coefficient (RC = 1.96 × SD of test-retest differences), linear regression analysis, and the intra-class correlation coefficient (ICC). The impact of different lesion selection criteria was also evaluated.
Images from four cohorts containing 30 patients with 52 lesions were obtained and analyzed (ten in breast cancer, nine in head and neck squamous cell carcinoma, and 33 in non-small cell lung cancer patients). A good correlation was found between test-retest data for all F-FLT uptake metrics (R ≥ 0.93; ICC ≥ 0.96). Best repeatability was found for SUV (RC: 23.1%), without significant differences in RC between different SUV metrics. Repeatability of proliferative volume (RC: 36.0%) and TLU (RC: 36.4%) was worse than SUV. Lesion selection methods based on SUV ≥ 4.0 improved the repeatability of volumetric metrics (RC: 26-28%), but did not affect the repeatability of SUV metrics.
In multi-center studies, differences ≥ 25% in F-FLT SUV metrics likely represent a true change in tumor uptake. Larger differences are required for FLT metrics comprising volume estimates when no lesion selection criteria are applied.
3'-去氧-3'-[F]氟代胸苷(F-FLT)正电子发射断层扫描(PET)提供了一种非侵入性的方法来评估细胞增殖和抗肿瘤治疗的反应。定量 F-FLT 摄取指标正在用于评估研究中的增殖反应,但是需要建立多中心的可重复性。本研究的目的是通过使用相同的肿瘤分割方法和重复性指标重新分析先前发表的报告中的个体患者数据,确定 F-FLT 肿瘤摄取指标的重复性。
从 1997 年 1 月至 2016 年 10 月,在 PubMed、EMBASE.com 和 Cochrane 图书馆进行了系统检索,共获得了五个实体瘤的 F-FLT 重复性队列。使用适用于测试和再测试扫描的局部背景的 50%等浓度线来描绘 F-FLT 阳性病灶。计算 SUV、SUV、SUV、增殖体积和总病灶摄取量(TLU)。使用重复性系数(RC=测试-复测差异的 1.96×SD)、线性回归分析和组内相关系数(ICC)评估重复性。还评估了不同病变选择标准的影响。
获得并分析了来自四个包含 30 例 52 个病变的患者的图像(乳腺癌 10 例,头颈部鳞状细胞癌 9 例,非小细胞肺癌患者 33 例)。所有 F-FLT 摄取指标的测试-复测数据之间均存在良好的相关性(R≥0.93;ICC≥0.96)。SUV 的重复性最好(RC:23.1%),不同 SUV 指标的 RC 无显著差异。增殖体积(RC:36.0%)和 TLU(RC:36.4%)的重复性不如 SUV。基于 SUV≥4.0 的病变选择方法改善了体积指标的重复性(RC:26-28%),但对 SUV 指标的重复性没有影响。
在多中心研究中,F-FLT SUV 指标的差异≥25%可能代表肿瘤摄取的真实变化。当不应用病变选择标准时,包含体积估计的 FLT 指标需要更大的差异。
Zotero 插件
