粒细胞集落刺激因子对淋巴瘤患者F-FDG生物分布影响的综合分析:对PET/CT检查安排的启示
Comprehensive analysis of the influence of G-CSF on the biodistribution of F-FDG in lymphoma patients: insights for PET/CT scheduling.
作者信息
Oliveira Magno, Lasnon Charline, Nganoa Catherine, Gac Anne-Claire, Damaj Gandhi, Aide Nicolas
机构信息
Nuclear Medicine Department, CHU de Caen, Caen, France.
Nuclear Medicine Department, Centre François Baclesse, Caen, France.
出版信息
EJNMMI Res. 2019 Aug 20;9(1):79. doi: 10.1186/s13550-019-0546-1.
AIMS
(1) To perform a comprehensive analysis of the time elapsed between the last G-CSF injection and the PET/CT examination on the biodistribution of F-FDG, with emphasis on liver, spleen, and bone marrow uptake, and (2) to investigate whether an inversion of the liver to spleen ratio affects the Deauville scoring.
MATERIALS AND METHODS
Retrospectively included were 74 consecutive diffuse large B cell lymphoma (DLBCL) patients referred for baseline and interim examinations and receiving immunochemotherapy with various G-CSF regimens. A comprehensive evaluation considering baseline metabolic active tumour volume (MATV), factors affecting liver uptake, the type of G-CSF, and the time elapsed between chemotherapy/G-CSF and interim PET/CTs was performed.
RESULTS
Mean (± SD) percentage variations between baseline and interim PET/CTs (i-PET/CT) for bone marrow (%Variation_), liver (%Variation_) and spleen (%Variation_) were equal to 32.0 ± 46.9%, 16.1 ± 42.8%, and 10.6 ± 51.1 %, respectively. %Variation_ and %Variation_ were higher in patients using lenograstim, but this was linked to lower uptakes at baseline and was therefore likely not due to G-CSF itself. The mean delay between G-CSF injection and i-PET/CT acquisition was not an independent explanatory variable for %Variation_, %Variation_, and %Variation_. On the contrary, %Variation_ and %Variation_ were negatively correlated to the time-lapse between the end of chemotherapy and i-PET/CT: ρ = - 0.342 (p = 0.010) and ρ = - 0.529 (p < 0.0001), respectively. Patients with a time-lapse since the last injection of chemotherapy < 17 days displayed higher bone and spleen SUVmax. %Variation_ was positively correlated to baseline MATV: ρ = 0.243 (p = 0.039). Patients displaying a high baseline MATV ≥ 177 cc had significantly lower liver SUVmax at baseline. This difference was no longer observed at i-PET/CT, after tumours had shrunk.
CONCLUSIONS
Neither the type of G-CSF used nor the time elapsed between its last injection and i-PET/CT examination independently influences bone, hepatic, or splenic uptakes at i-PET/CT. The major determinant for the occurrence of a bone or spleen hypermetabolism on i-PET/CT is the time elapsed between the chemotherapy and the examination, which should be maintained above 15 days. Inversion of the liver to spleen ratio appeared to be due to increased spleen hypermetabolism on i-PET/CT, making unlikely an impact on the Deauville scoring.
目的
(1)全面分析末次注射粒细胞集落刺激因子(G-CSF)至正电子发射断层显像/计算机断层扫描(PET/CT)检查之间的时间间隔对氟代脱氧葡萄糖(F-FDG)生物分布的影响,重点关注肝脏、脾脏和骨髓摄取情况;(2)研究肝脾比值倒置是否会影响多维尔评分。
材料与方法
回顾性纳入74例连续的弥漫性大B细胞淋巴瘤(DLBCL)患者,这些患者接受基线和中期检查,并采用不同的G-CSF方案进行免疫化疗。综合评估考虑了基线代谢活性肿瘤体积(MATV)、影响肝脏摄取的因素、G-CSF的类型以及化疗/G-CSF与中期PET/CT之间的时间间隔。
结果
基线与中期PET/CT(i-PET/CT)之间骨髓(%变化_)、肝脏(%变化_)和脾脏(%变化_)的平均(±标准差)百分比变化分别为32.0±46.9%、16.1±42.8%和10.6±51.1%。使用来格司亭的患者%变化_和%变化_较高,但这与基线时较低的摄取有关,因此可能不是由于G-CSF本身。G-CSF注射与i-PET/CT采集之间的平均延迟不是%变化_、%变化_和%变化_的独立解释变量。相反,%变化_和%变化_与化疗结束至i-PET/CT的时间间隔呈负相关:ρ=-0.342(p=0.010)和ρ=-0.529(p<0.0001)。自末次化疗注射以来时间间隔<17天的患者显示出更高的骨骼和脾脏最大标准摄取值(SUVmax)。%变化_与基线MATV呈正相关:ρ=0.243(p=0.039)。基线MATV≥177 cc的高基线患者在基线时肝脏SUVmax显著较低。肿瘤缩小后,在i-PET/CT时未再观察到这种差异。
结论
所使用的G-CSF类型及其末次注射与i-PET/CT检查之间的时间间隔均不会独立影响i-PET/CT时骨骼、肝脏或脾脏的摄取。i-PET/CT上骨骼或脾脏代谢亢进发生的主要决定因素是化疗与检查之间的时间间隔,该间隔应保持在15天以上。肝脾比值倒置似乎是由于i-PET/CT上脾脏代谢亢进增加所致,不太可能对多维尔评分产生影响。
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