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复发性和转移性乳腺癌的PET、PET/CT、PET/MRI:氟代脱氧葡萄糖及新生物标志物

Recurrent and metastatic breast cancer PET, PET/CT, PET/MRI: FDG and new biomarkers.

作者信息

Gaeta C M, Vercher-Conejero J L, Sher A C, Kohan A, Rubbert C, Avril N

机构信息

University Hospitals Case Medical Center Case Western Reserve University, Cleveland, OH, USA -

出版信息

Q J Nucl Med Mol Imaging. 2013 Dec;57(4):352-66.

PMID:24322792
Abstract

Primary breast cancer often displays only moderately increased glucose metabolism resulting in a low sensitivity of positron emission tomography (PET) using [F-18]fluorodeoxyglucose (FDG) in detecting small breast carcinomas, locoregional micrometastases and non-enlarged tumor infiltrated lymphnodes. In contrast, distant breast cancer metastases are generally characterized by significantly increased metabolic activity compared to normal tissue. Therefore, FDG-PET provides accurate diagnostic information as a whole body imaging modality in staging of breast cancer patients. The metabolic information from FDG-PET/CT is often more sensitive than conventional imaging for the detection of distant metastases, particularly in the recurrent setting. FDG-PET is superior in detecting tumor-involved distant lymphnodes, particularly those which are normal in size, as well as in characterizing enlarged lymphnodes as positive or negative for malignancy. Of note, CT is superior in detecting small lung metastases. Although the overall sensitivity for bone scintigraphy and FDG-PET are comparable, bone scintigraphy seems to be superior in the detection of osteoblastic disease whereas FDG-PET is superior for osteolytic metastases, suggesting a complementary role for both imaging procedures. FDG-PET/MR has an evolving role in breast cancer management, for example in the detection of liver metastases and in the research setting for treatment monitoring. The utilization of PET for prediction of treatment response to primary chemotherapy is an area of active research, using FDG as well as other PET biomarkers including [F-18]Fluoroestradiol, [F-18]Fluorothymidine and integrin targeting tracer for monitoring anti-angiogenic therapy.

摘要

原发性乳腺癌通常仅表现出适度增加的葡萄糖代谢,这导致使用[F-18]氟脱氧葡萄糖(FDG)的正电子发射断层扫描(PET)在检测小乳腺癌、局部区域微转移和未增大的肿瘤浸润淋巴结时灵敏度较低。相比之下,远处乳腺癌转移灶的代谢活性通常明显高于正常组织。因此,FDG-PET作为一种全身成像方式,在乳腺癌患者分期中可提供准确的诊断信息。FDG-PET/CT的代谢信息在检测远处转移方面通常比传统成像更敏感,尤其是在复发情况下。FDG-PET在检测肿瘤累及的远处淋巴结方面具有优势,特别是那些大小正常的淋巴结,以及在将增大的淋巴结区分为恶性阳性或阴性方面。值得注意的是,CT在检测小肺转移方面更具优势。虽然骨闪烁显像和FDG-PET的总体灵敏度相当,但骨闪烁显像在检测成骨性病变方面似乎更具优势,而FDG-PET在检测溶骨性转移方面更具优势,这表明两种成像方法具有互补作用。FDG-PET/MR在乳腺癌管理中发挥着越来越重要的作用,例如在检测肝转移以及在治疗监测的研究环境中。利用PET预测对原发性化疗的治疗反应是一个活跃的研究领域,使用FDG以及其他PET生物标志物,包括[F-18]氟雌二醇、[F-18]氟胸腺嘧啶和整合素靶向示踪剂来监测抗血管生成治疗。

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