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正电子发射断层扫描技术(PET)成像中的嘧啶类增殖研究

PET imaging of proliferation with pyrimidines.

机构信息

Department of Oncology, Karmanos Cancer Institute, Wayne State University, Detroit, Michigan 48201, USA.

出版信息

J Nucl Med. 2013 Jun;54(6):903-12. doi: 10.2967/jnumed.112.112201. Epub 2013 May 14.

DOI:10.2967/jnumed.112.112201
PMID:23674576
Abstract

Several new tracers are being developed for use with PET to assess pathways that are altered in cancers, including energy use, cellular signaling, transport, and proliferation. Because increased proliferation is a hallmark of many cancers, several tracers have been tested to track the DNA synthesis pathway. Thymidine, which is incorporated into DNA but not RNA, has been used in laboratory studies to measure tumor growth. Because thymidine labeled with (11)C undergoes rapid biologic degradation and has a short physical half-life, tracers labeled with (18)F have been preferred in PET imaging. One such tracer is (18)F-labeled 3'-deoxy-3'-fluorothymidine ((18)F-FLT). (18)F-FLT is trapped after phosphorylation by thymidine kinase 1, whose expression is increased in replicating cells. Several studies on breast, lung, and brain tumors have demonstrated that retention of (18)F-FLT correlated with tumor proliferation. Although (18)F-FLT has been used to image and stage several tumor types, the standardized uptake value is generally lower than that obtained with (18)F-FDG. (18)F-FLT can be used to image many areas of the body, but background uptake is high in the liver, marrow, and renal system, limiting use in these organs. (18)F-FLT PET imaging has primarily been studied in the assessment of treatment response. Rapid declines in (18)F-FLT retention within days to weeks have been demonstrated in several tumor types treated with cytotoxic drugs, targeted agents, and radiotherapy. Further work is ongoing to validate this approach and determine its utility in the development of new drugs and in the clinical evaluation of standard treatment approaches.

摘要

几种新的示踪剂正在开发中,用于 PET 以评估癌症中改变的途径,包括能量利用、细胞信号转导、运输和增殖。由于增殖增加是许多癌症的标志,因此已经测试了几种示踪剂来跟踪 DNA 合成途径。胸腺嘧啶核苷不掺入 RNA 但掺入 DNA,已在实验室研究中用于测量肿瘤生长。由于标记有 (11)C 的胸腺嘧啶核苷迅速进行生物降解并且具有短的物理半衰期,因此在 PET 成像中更喜欢标记有 (18)F 的示踪剂。一种这样的示踪剂是 (18)F 标记的 3'-去氧-3'-氟胸苷 ((18)F-FLT)。(18)F-FLT 在磷酸化后被胸苷激酶 1 捕获,其表达在复制细胞中增加。几项关于乳腺癌、肺癌和脑肿瘤的研究表明,(18)F-FLT 的保留与肿瘤增殖相关。尽管 (18)F-FLT 已被用于成像和分期几种肿瘤类型,但标准化摄取值通常低于 (18)F-FDG 获得的值。(18)F-FLT 可用于成像身体的许多部位,但肝脏、骨髓和肾脏系统的背景摄取较高,限制了在这些器官中的使用。(18)F-FLT PET 成像主要在评估治疗反应方面进行了研究。在几种用细胞毒性药物、靶向药物和放射治疗治疗的肿瘤类型中,已经证明在几天到几周内 (18)F-FLT 保留迅速下降。正在进行进一步的工作来验证这种方法并确定其在新药开发和标准治疗方法的临床评估中的效用。

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