Fuster D, Ayuso J R, Poveda A, Cubedo R, Casado A, Martínez-Trufero J, López-Pousa A, Del Muro X G, Lomeña F, Maurel J, Pons F
Nuclear Medicine, Hospital Clínic Barcelona, Barcelona, Spain.
Q J Nucl Med Mol Imaging. 2011 Dec;55(6):680-7. Epub 2010 Dec 9.
The aim of this study was to evaluate the utility of positron emission tomography with 18F-fluorodeoxyglucose (FDG-PET) in monitoring response in refractory GIST.
This multicenter study prospectively evaluated 21 patients with locally advanced and/or metastatic GIST refractory to with high-dose imatinib (800 mg/day) treated with doxorubicin 15-20 mg/m2/weekly for 4 cycles, followed by imatinib maintenance (400 mg/day). CT and FDG-PET were performed at baseline and after completion of therapy.
Mean baseline tumor size on CT was 5.9 cm. Median progression-free survival (PFS) was 219 days (range 62-1108). Three out of 21 patients (14%) had partial responses (PR) under RECIST criteria, 12 patients (57%) remained stable (SD) and 6 showed progression (PD) of the disease during treatment (29%). Six patients had PR by FDG-PET, 15 showed SD (n=9) or PD (n=6) based on EORTC criteria. Patients with a PFS <6 mo showed a significantly higher ∑SUVmax at baseline (26.04±13.4) than those with PFS≥6 mo (9.82±5.0) (P<0.05). A correlation was found between PET response and PFS: PR 14±6.1 mo, SD 5.5±0.8 mo and PD 3.5±4.1 mo (P<0.05). A residual SUVmax <5 after treatment correlated with improved PFS (314±315 days vs 131±91 days) (P<0.01). Survival curves showed a significant association between PET response and PFS (P<0.05). Patients with wild-type genotype KIT (KIT-WT) showed a significantly lower baseline SUVmax (5.36±1.4) than non-WT KIT (8.40±3.6) (P<0.05).
FDG-PET is useful in assessing response of GIST refractory to imatinib and correlates with the presence of KIT-WT. Baseline ∑SUVmax can predict response to treatment in this series.
本研究旨在评估18F-氟脱氧葡萄糖正电子发射断层扫描(FDG-PET)在监测难治性胃肠间质瘤(GIST)反应中的效用。
这项多中心研究前瞻性评估了21例局部晚期和/或转移性GIST患者,这些患者对高剂量伊马替尼(800mg/天)耐药,接受阿霉素15-20mg/m²/周治疗4个周期,随后进行伊马替尼维持治疗(400mg/天)。在基线期和治疗结束后进行CT和FDG-PET检查。
CT上的平均基线肿瘤大小为5.9cm。中位无进展生存期(PFS)为219天(范围62-1108天)。根据RECIST标准,21例患者中有3例(14%)出现部分缓解(PR),12例(57%)病情稳定(SD),6例在治疗期间病情进展(PD)(29%)。根据FDG-PET,6例患者出现PR,15例根据欧洲癌症研究与治疗组织(EORTC)标准显示为SD(n=9)或PD(n=6)。PFS<6个月的患者在基线时的∑SUVmax(26.⒈04±13.4)显著高于PFS≥6个月患者(9.82±5.0)(P<0.05)。发现PET反应与PFS之间存在相关性:PR为14±6.1个月,SD为5.5±0.8个月,PD为3.5±4.1个月(P<0.05)。治疗后残余SUVmax<5与PFS改善相关(314±315天对131±91天)(P<0.01)。生存曲线显示PET反应与PFS之间存在显著关联(P<0.05)。野生型KIT基因型(KIT-WT)患者的基线SUVmax(5.36±1.4)显著低于非WT KIT患者(8.40±3.6)(P<0.05)。
FDG-PET有助于评估对伊马替尼耐药的GIST的反应,并与KIT-WT的存在相关。基线∑SUVmax可预测本系列患者的治疗反应。
