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正电子发射断层扫描与骨转移

Positron emission tomography and bone metastases.

作者信息

Fogelman Ignac, Cook Gary, Israel Ora, Van der Wall Hans

机构信息

Division of Imaging, King's College, London, United Kingdom.

出版信息

Semin Nucl Med. 2005 Apr;35(2):135-42. doi: 10.1053/j.semnuclmed.2004.11.005.

Abstract

The use of 2-[18F]fluoro-2-deoxy-D-glucose positron emission tomography (FDG-PET) in the evaluation and management of patients with malignancy continues to increase. However, its role in the identification of bone metastases is far from clear. FDG has the advantage of demonstrating all metastatic sites, and in the skeleton it is assumed that its uptake is directly into tumor cells. It is probable that for breast and lung carcinoma, FDG-PET has similar sensitivity, although poorer specificity, when compared with the isotope bone scan, although there is conflicting evidence, with several articles suggesting that it is less sensitive than conventional imaging in breast cancer. There is convincing evidence that for prostate cancer, FDG-PET is less sensitive than the bone scan and this may be tumor specific. There is very little data relating to lymphoma, but FDG-PET seems to perform better than the bone scan. There is an increasing body of evidence relating to the valuable role of FDG-PET in myeloma, where it is clearly better than the bone scan, presumably because FDG is identifying marrow-based disease at an early stage. There are, however, several other important variables that should be considered. The morphology of the metastasis itself appears to be relevant. At least in breast cancer, different patterns of FDG uptake have been shown in sclerotic, lytic, or lesions with a mixed pattern, Furthermore, the precise localization of a metastasis in the skeleton may be important with regard to the extent of the metabolic response induced. Previous treatment is highly relevant and it has been found that although the majority of untreated bone metastases are positive on PET scans and have a lytic pattern on computed tomography (CT), after treatment, incongruent CT-positive/PET-negative lesions are significantly more prevalent and generally are blastic, which presumably reflects a direct effect of treatment. Finally, the aggressiveness of the tumor itself may be relevant. The most important question, however, is irrespective of whether a lesion is seen on x-ray, CT, or bone scan and irrespective of lytic of blastic morphology: if the FDG-PET study is negative, what is the clinical relevance of that lesion?

摘要

2-[18F]氟-2-脱氧-D-葡萄糖正电子发射断层扫描(FDG-PET)在恶性肿瘤患者的评估和管理中的应用持续增加。然而,其在骨转移瘤识别中的作用尚不清楚。FDG的优势在于能显示所有转移部位,在骨骼中,其摄取被认为是直接进入肿瘤细胞。对于乳腺癌和肺癌,与同位素骨扫描相比,FDG-PET可能具有相似的敏感性,尽管特异性较差,不过也有相互矛盾的证据,有几篇文章表明它在乳腺癌中比传统成像的敏感性更低。有令人信服的证据表明,对于前列腺癌,FDG-PET比骨扫描敏感性更低,这可能具有肿瘤特异性。关于淋巴瘤的数据非常少,但FDG-PET似乎比骨扫描表现更好。越来越多的证据表明FDG-PET在骨髓瘤中具有重要作用,在骨髓瘤中它明显优于骨扫描,大概是因为FDG能在早期识别基于骨髓的疾病。然而,还有其他几个重要变量需要考虑。转移瘤本身的形态似乎很重要。至少在乳腺癌中,在硬化性、溶解性或混合性病变中已显示出不同的FDG摄取模式。此外,转移瘤在骨骼中的精确定位对于诱导的代谢反应程度可能很重要。先前的治疗高度相关,并且已发现尽管大多数未经治疗的骨转移瘤在PET扫描上呈阳性且在计算机断层扫描(CT)上呈溶解性模式,但治疗后,CT阳性/PET阴性的不一致病变更为普遍,并且通常是成骨性的,这大概反映了治疗的直接作用。最后,肿瘤本身的侵袭性可能也有关系。然而,最重要的问题是,无论病变在X线、CT或骨扫描上是否可见,也无论其溶解性或成骨性形态如何:如果FDG-PET检查为阴性,该病变的临床意义是什么?

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