首页> 外文期刊>European Journal of Nuclear Medicine and Molecular Imaging >Lesion-based detection of early chemosensitivity using serial static FDG PET/CT in metastatic colorectal cancer.
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Lesion-based detection of early chemosensitivity using serial static FDG PET/CT in metastatic colorectal cancer.

机译:在转移性大肠癌中使用系列静态FDG PET / CT基于病变的早期化学敏感性检测。

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Medical oncology needs early identification of patients that are not responding to systemic therapy. (18)F-Fluorodeoxyglucose (FDG) positron emission tomography (PET) performed before and early during treatment has been proposed for this purpose. However, the best way to assess the change in FDG uptake between two scans has not been identified. We studied cutoff thresholds to identify responding tumours as a function of the method used to measure tumour uptake.The study included 28 metastatic colorectal cancer (mCRC) patients who underwent 2 FDG PET/CT scans (baseline and at day 14 of the first course of polychemotherapy). For 78 tumour lesions, 4 standardized uptake value (SUV) indices were measured: maximum SUV (SUV(max)) and mean SUV in a region obtained using an isocontour (SUV(40 %)), with each of these SUV normalized either by the patient body weight (BW) or body surface area (BSA). The per cent change and absolute change in tumour uptake between the baseline and the early PET scans were measured based on these four indices. These changes were correlated to the RECIST 1.0-based response using contrast-enhanced CT at baseline and at 6-8 weeks on treatment.The 78 tumours were classified as non-responding (NRL, n = 58) and responding lesions (RL, n = 20). Receiver-operating characteristic (ROC) curves characterizing the performance in NRL/RL classification using early FDG PET uptake had areas under the curve between 0.75 and 0.84, without significant difference between the indices. The cutoff threshold in FDG uptake per cent change to get a 95 % sensitivity of RL detection depended on the way uptake was measured: -14 % (specificity of 53 %) and -22 % (specificity of 64 %) for SUV(max) and SUV(40 %), respectively. Thresholds expressed as absolute SUV decrease instead of per cent change were less sensitive to the SUV definition: an SUV decline by 1.2 yielded a sensitivity of RL detection of 95 % for SUV(max) and SUV(40 %). For a given cutoff threshold, the sensitivity was the same whatever the normalization (by BSA or BW).A 14 % drop of tumour FDG SUV(max), 22 % drop of SUV(40 %) or 1.2 drop of SUV(max) or SUV(mean) after one single course of polychemotherapy predicts objective response in mCRC lesions with a high sensitivity, potentially allowing the early identification of non-responding patients.
机译:医学肿瘤学需要及早发现对全身治疗无反应的患者。为此,已经提出了在治疗之前和治疗初期进行的(18)F-氟脱氧葡萄糖(FDG)正电子发射断层显像(PET)。但是,尚未确定评估两次扫描之间FDG吸收变化的最佳方法。我们研究了临界阈值,以根据测量肿瘤吸收的方法确定反应性肿瘤。该研究包括28位转移性结直肠癌(mCRC)患者,他们接受了2次FDG PET / CT扫描(基线和第一疗程的第14天)多化学疗法)。对于78个肿瘤病变,测量了4个标准化摄取值(SUV)指数:最大SUV(SUV(max))和使用等高线获得的区域中的平均SUV(SUV(40%)),这些SUV均通过患者体重(BW)或身体表面积(BSA)。基于这四个指标,测量了基线和早期PET扫描之间肿瘤吸收的百分比变化和绝对变化。这些变化与基线和治疗6-8周时使用对比增强CT的基于RECIST 1.0的反应相关.78例肿瘤被分类为无反应(NRL,n = 58)和有反应的病变(RL,n = 20)。使用早期FDG PET摄取表征NRL / RL分类性能的接收者操作特征(ROC)曲线的曲线下面积在0.75至0.84之间,指标之间无显着差异。达到95%RL检测灵敏度的FDG吸收百分比变化的临界阈值取决于测量的吸收方式:SUV(max)为-14%(特异性为53%)和-22%(特异性为64%)。和SUV(分别为40%)。表示为SUV绝对下降而不是百分比变化的阈值对SUV定义不太敏感:SUV下降1.2时,对于SUV(最大)和SUV(40%)的RL检测灵敏度为95%。对于给定的截断阈值,无论标准化(通过BSA或BW),灵敏度都相同。肿瘤FDG SUV(最大)下降14%,SUV(22%)下降40%(SUV)(最大)22%单一化学疗法疗程后的SUV(平均)或SUV(均值)预测mCRC病变的客观反应具有很高的敏感性,可能允许及早识别出无反应的患者。

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