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肿瘤学实践中的非FDG正电子发射断层显像

Non-FDG PET in the practice of oncology.

作者信息

Caroli P, Nanni C, Rubello D, Alavi A, Fanti S

机构信息

Nuclear Medicine, University of Bologna, Bologna, Italy.

出版信息

Indian J Cancer. 2010 Apr-Jun;47(2):120-5. doi: 10.4103/0019-509X.62998.

Abstract

Fluoro-2-deoxy-D-glucose-positron emission tomography (FDG-PET) is utilized in more than 90% of cancers in staging, re-staging, assessing therapy response and during the follow-up. However, not all tumors show significant increase of metabolic activity on FDG-PET imaging. This is particularly true for prostate cancer, neuroendocrine tumors and hepatic tumors. In this review we have considered those already used for clinical applications such as 11C- and 18F-Choline, 11C-Methionine and 18F-FET, 18F-DOPA, 68Ga-DOTA-somatostatine analogues, 11C-Acetate and 18F-FLT. Choline presents a high affinity for malignant prostate tissue, even if low grade. Choline can be labeled with either 11C or 18F, the former being the preference due to lower urinary excretion and patients exposure. The latter is more useful for possible distribution to centers lacking in on-site cyclotron. Methionine is needed for protein synthesis and tumor cells require an external supply of methionine. These tracers have primarily been used for imaging of CNS neoplasms. The most appropriate indication is when conventional imaging procedures do not distinguish between edema, fibrosis or necrosis and disease relapse. In addition, the uptake of 11C-Methionine is proportional to the tumor grade and, therefore, the maximum small unilamellar vesicles (SUV) inside the brain mass before therapy is somehow considered a prognostic value. Neuroendocrine tumors (carcinoids, pheocromocytoma, neuroblastoma, medullary thyroid cancer, microcytoma, carotid glomus tumors, and melanoma) demonstrate an increased activity of L-DOPA decarboxylase, and hence they show a high uptake of 18FDOPA. For the study of NETs, 68Ga-DOTA-TOC/DOTA-NOC has been introduced as PET tracer. This compound for PET imaging has a high affinity for sst2 and sst5 and has been used in the detection of NETs in preliminary studies; 68Ga-DOTA-NOC PET is useful before metabolic radiotherapy in order to evaluate the biodistribution of the therapeutic compound; 18F-FLT is a specific marker of cell proliferation and the most important field of application of FLT is lung cancer. Other tracers are used in PET utilized as markers of hypoxia inside big neoplastic masses include 18F-MISO, 64Cu-ATSM, 18F-EF5, which highlight the presence of hypoxic areas are useful for patients that must be treated with radiotherapy.

摘要

氟代 - 2 - 脱氧 - D - 葡萄糖正电子发射断层扫描(FDG - PET)在90%以上的癌症分期、再分期、评估治疗反应及随访过程中被使用。然而,并非所有肿瘤在FDG - PET成像上都显示代谢活性显著增加。前列腺癌、神经内分泌肿瘤和肝肿瘤尤其如此。在本综述中,我们考虑了那些已用于临床应用的示踪剂,如11C - 和18F - 胆碱、11C - 蛋氨酸和18F - FET、18F - DOPA、68Ga - DOTA - 生长抑素类似物、11C - 醋酸盐和18F - FLT。胆碱对恶性前列腺组织具有高亲和力,即使是低级别肿瘤。胆碱可用11C或18F标记,由于较低的尿液排泄和患者暴露,前者更受青睐。后者对于可能分发给缺乏现场回旋加速器的中心更有用。蛋氨酸是蛋白质合成所必需的,肿瘤细胞需要外部供应蛋氨酸。这些示踪剂主要用于中枢神经系统肿瘤的成像。最合适的适应症是当传统成像程序无法区分水肿、纤维化或坏死与疾病复发时。此外,11C - 蛋氨酸的摄取与肿瘤分级成正比,因此,治疗前脑肿瘤内的最大标准化摄取值(SUV)在某种程度上被视为一种预后价值。神经内分泌肿瘤(类癌、嗜铬细胞瘤、神经母细胞瘤、甲状腺髓样癌、微细胞瘤、颈动脉体瘤和黑色素瘤)表现出L - DOPA脱羧酶活性增加,因此它们对18F - DOPA摄取较高。对于神经内分泌肿瘤的研究,68Ga - DOTA - TOC/DOTA - NOC已作为PET示踪剂引入。这种用于PET成像的化合物对sst2和sst5具有高亲和力,并已在初步研究中用于神经内分泌肿瘤的检测;68Ga - DOTA - NOC PET在代谢放疗前用于评估治疗化合物的生物分布;18F - FLT是细胞增殖的特异性标志物,FLT最重要的应用领域是肺癌。其他示踪剂在PET中用作大肿瘤块内缺氧的标志物,包括18F - MISO、64Cu - ATSM、18F - EF5,它们突出缺氧区域的存在,对必须接受放疗的患者有用。

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