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甲硫氨酸和 PBR28 作为 PET 成像示踪剂,以区分转移性肿瘤复发或放射性坏死。

[C]Methionine and [C]PBR28 as PET Imaging Tracers to Differentiate Metastatic Tumor Recurrence or Radiation Necrosis.

机构信息

Yale School of Medicine and Yale Cancer Center, 12228Yale University, New Haven, CT, USA.

Department of Radiology and Biomedical Imaging, Yale School of Medicine, 12228Yale University, New Haven, CT, USA.

出版信息

Mol Imaging. 2020 Jan-Dec;19:1536012120968669. doi: 10.1177/1536012120968669.

Abstract

PURPOSE

As stereotactic radiosurgery (SRS) and immunotherapy are increasingly used to treat brain metastases, incidence of radiation necrosis (RN) is consequently rising. Differentiating tumor regrowth (TR) from RN is vital in management but difficult to assess using MRI. We hypothesized that tumor methionine levels would be elevated given increased metabolism and high amino acid uptake, whereas RN would increase inflammation marked by upregulated translocator protein (PBR-TSPO), which can be quantified with specific PET tracers.

PROCEDURES

We performed a feasibility study to prospectively evaluate [C]methionine and [C]PBR28 using PET in 5 patients with 7 previously SRS-treated brain metastases demonstrating regrowth to differentiate TR from RN.

RESULTS

Sequential imaging with dual tracers was well-tolerated. [C]methionine was accurate for detecting pathologically confirmed TR in 7/7 lesions, whereas [C]PBR28 was only accurate in 3/7 lesions. Tumor PBR-TSPO expression was elevated in both melanoma and lung cancer cells, contributing to lack of specificity of [C]PBR28-PET.

CONCLUSION

Sequential use of PET tracers is safe and effective. [C]Methionine was a reliable TR marker, but [C]PBR28 was not a reliable marker of RN. Studies are needed to determine the causes of post-radiation inflammation and identify specific markers of RN to improve diagnostic imaging.

摘要

目的

随着立体定向放射外科(SRS)和免疫疗法越来越多地用于治疗脑转移瘤,放射性坏死(RN)的发病率也随之上升。区分肿瘤复发(TR)和放射性坏死对于管理至关重要,但使用 MRI 评估较为困难。我们假设,由于代谢增加和氨基酸摄取增加,肿瘤蛋氨酸水平会升高,而放射性坏死会增加炎症,炎症表现为转位蛋白(PBR-TSPO)上调,这可以用特定的 PET 示踪剂来定量。

程序

我们进行了一项可行性研究,前瞻性评估了 5 名患者的 7 个之前接受 SRS 治疗的脑转移瘤,这些转移瘤出现生长以区分 TR 和 RN,使用 [C]蛋氨酸和 [C]PBR28 进行 PET。

结果

双重示踪剂的连续成像耐受性良好。[C]蛋氨酸在 7/7 例经病理证实的 TR 检测中准确,而 [C]PBR28 仅在 3/7 例中准确。黑色素瘤和肺癌细胞中肿瘤 PBR-TSPO 表达升高,导致 [C]PBR28-PET 特异性差。

结论

顺序使用 PET 示踪剂是安全有效的。[C]蛋氨酸是可靠的 TR 标志物,但 [C]PBR28 不是 RN 的可靠标志物。需要进一步研究以确定放射性炎症的原因,并确定 RN 的特异性标志物,以改善诊断成像。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f1ce/7649862/0b331ee23f69/10.1177_1536012120968669-fig1.jpg

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