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评估男性患者中11C-胆碱、18F-甲基胆碱和18F-乙基胆碱前列腺外摄取情况的多中心研究:生理分布、统计学差异、影像要点及正常变异

Multicenter study evaluating extraprostatic uptake of 11C-choline, 18F-methylcholine, and 18F-ethylcholine in male patients: physiological distribution, statistical differences, imaging pearls, and normal variants.

作者信息

Haroon Athar, Zanoni Lucia, Celli Monica, Zakavi Rasoul, Beheshti Mohsen, Langsteger Werner, Fanti Stefano, Emberton Mark, Bomanji Jamshed

机构信息

aDepartment Institute of Nuclear Medicine, T5 University College Hospital, London, UK bDepartment of Nuclear Medicine, University Hospital Sant'Orsola Malpighi, Bologna, Italy cNuclear Medicine Research Center, Mashad University of Medical Sciences, Mashhad, Iran dSt Vincent's Hospital, Linz, Austria.

出版信息

Nucl Med Commun. 2015 Nov;36(11):1065-75. doi: 10.1097/MNM.0000000000000372.

Abstract

AIM

The aim of the study was to evaluate the visceral localization of the three most commonly used choline-based radiotracers (C-choline, F-methylcholine, and F-ethylcholine) with the aim of analyzing uptake in metabolically and anatomically disease-free patients.

MATERIALS AND METHODS

A total of 1250 standardized uptake values (SUVmax, SUVmean) were analyzed in 45 anatomical regions in 45 patients (15 patients with C-choline, 15 with F-methylcholine, and 15 with F-ethylcholine). These patients were selected from a cohort of 3721 choline PET/computed tomography studies performed at three teaching hospitals over a period of 10 years. They had no evidence of metabolically active primary disease, metastatic disease, or altered morphology on the computed tomography component of the study or any evidence of disease elsewhere on other imaging modalities. The sites of primary disease (prostate and seminal vesicles) were excluded from evaluation.

RESULTS

No adverse effect was documented when using the three tracers. Visceral localization was the same for all three tracers. Viscera with a statistical difference in intensity of uptake included the choroid plexus (P=0.0001), occipital lobe (P=0.014), parietal lobe (P=0.008), cerebellum (P=0.003), parotid gland (P=0.005), submandibular gland (P=0.001), tonsils (P=0.001), thyroid (P=0.0001), lungs (P=0.001), aorta (P=0.001), pulmonary artery (P=0.0001), liver segments I (P=0.005), III (P=0.005), IVB (P=0.03), and V (P=0.01), spleen [hilum (P=0.0009), body (P=0.0001)], pancreas [head (P=0.0001), body (P=0.01), tail (P=0.002)], esophagus (P=0.001), stomach (P=0.0001), duodenum (P=0.0002), large intestine (P=0.008), and rectum (P=0.0001). Elsewhere, no statistical difference was observed. Excreted activity was noted in the kidneys and bladder.

CONCLUSION

This study demonstrates that the visceral localization of C-choline, F-methylcholine, and F-ethylcholine in disease-free patients is similar. Depending on the tracer uptake pattern, the viscera can be divided into two distinct categories: those with a statistically significant difference in uptake and those with no difference in uptake. The study outlines the range of SUVs for various organs for the three tracers and identifies some of the potential pitfalls in the evaluation of 'nonavid' but clinically significant presentation of different disease entities.

摘要

目的

本研究旨在评估三种最常用的基于胆碱的放射性示踪剂(C - 胆碱、F - 甲基胆碱和F - 乙基胆碱)的内脏定位情况,分析其在代谢和解剖结构均无疾病的患者中的摄取情况。

材料与方法

对45例患者(15例使用C - 胆碱、15例使用F - 甲基胆碱、15例使用F - 乙基胆碱)的45个解剖区域的1250个标准化摄取值(SUVmax、SUVmean)进行分析。这些患者选自10年间在三家教学医院进行的3721例胆碱PET/计算机断层扫描研究队列。他们在研究的计算机断层扫描部分没有代谢活跃的原发性疾病、转移性疾病或形态改变的证据,也没有其他影像学检查显示其他部位有疾病的证据。原发性疾病部位(前列腺和精囊)被排除在评估之外。

结果

使用这三种示踪剂均未记录到不良反应。三种示踪剂的内脏定位相同。摄取强度有统计学差异的内脏包括脉络丛(P = 0.0001)、枕叶(P = 0.014)、顶叶(P = 0.008)、小脑(P = 0.003)、腮腺(P = 0.005)、下颌下腺(P = 0.001)、扁桃体(P = 0.001)、甲状腺(P = 0.0001)、肺(P = 0.001)、主动脉(P = 0.001)、肺动脉(P = 0.0001)、肝段I(P = 0.005)、III(P = 0.005)、IVB(P = 0.03)和V(P = 0.01)、脾脏[脾门(P = 0.0009)、脾体(P = 0.0001)]、胰腺[胰头(P = 0.0001)、胰体(P = 0.01)、胰尾(P = 0.002)]、食管(P = 0.001)、胃(P = 0.0001)、十二指肠(P = 0.0002)、大肠(P = 0.008)和直肠(P = 0.0001)。其他部位未观察到统计学差异。在肾脏和膀胱中观察到排泄活性。

结论

本研究表明,C - 胆碱、F - 甲基胆碱和F - 乙基胆碱在无疾病患者中的内脏定位相似。根据示踪剂摄取模式,内脏可分为两类:摄取有统计学显著差异的和摄取无差异的。该研究概述了三种示踪剂在各器官中的SUV范围,并确定了在评估不同疾病实体的“无摄取”但具有临床意义的表现时的一些潜在陷阱。

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