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使用镓标记的喷替沙氟(Pars-Cixafor™)PET/CT成像对高级别胶质瘤中趋化因子受体4(CXCR4)过表达进行的前瞻性评估。

A Prospective Evaluation of Chemokine Receptor-4 (CXCR4) Overexpression in High-grade Glioma Using Ga-Pentixafor (Pars-Cixafor™) PET/CT Imaging.

作者信息

Dadgar Habibollah, Norouzbeigi Nasim, Assadi Majid, Jafari Esmail, Al-Balooshi Batool, Al-Ibraheem Akram, Esmail Abdulredha A, Marafi Fahad, Haidar Mohamad, Al-Alawi Haider Muhsin, Omar Yehia, Usmani Sharjeel, Cimini Andrea, Ricci Maria, Arabi Hossein, Zaidi Habib

机构信息

Cancer Research Center, RAZAVI Hospital, Imam Reza International University, Mashhad, Iran (H.D., N.N.).

The Persian Gulf Nuclear Medicine Research Center, Department of Molecular Imaging and Radionuclide Therapy (MIRT), Bushehr Medical University Hospital, Bushehr University of Medical Sciences, Bushehr, Iran (M.A., E.J.).

出版信息

Acad Radiol. 2025 Apr;32(4):2247-2256. doi: 10.1016/j.acra.2024.11.064. Epub 2024 Dec 16.

Abstract

BACKGROUND

While magnetic resonance imaging (MRI) remains the gold standard for morphological imaging, its ability to differentiate between tumor tissue and treatment-induced changes on the cellular level is insufficient. Notably, glioma cells, particularly glioblastoma multiforme (GBM), demonstrate overexpression of chemokine receptor-4 (CXCR4). This study aims to evaluate the feasibility of non-invasive Ga-Cixafor™ PET/CT as a tool to improve diagnostic accuracy in patients with high-grade glioma.

METHODS

In this retrospective analysis, a database of histopathology-confirmed glioma patients with MRI findings consistent with high-grade gliomas was utilized. Within 2 weeks of their MRI, these patients underwent Ga-Cixafor™ PET/CT scans to assess CXCR4 expression. Both visual scoring based on established criteria and semi-quantitative measures including maximum standardized uptake value (SUV) and tumor-to-background ratios (TBR) were calculated to analyze the PET/CT data.

RESULTS

Our retrospective study enrolled 29 histologically confirmed glioma patients with MRI findings consistent with high-grade gliomas. All patients underwent Ga-Cixafor™ PET/CT scans within 2 weeks of their MRI, specifically at one-hour post-injection time point. Visual assessment based on a standardized scoring system identified 27 positive scans out of 29 (93.1%). Median SUV was 2.31 (range: 0.49-9.96) and median TBR was 20 (range: 6.12-124.5). Pathological analysis revealed 5 grade III (17.24%) and 24 grade IV (82.75%) lesions among the 29 patients. Notably, the median SUV of grade IV lesions (2.85) was significantly higher than grade III lesions (1.27) (P=0.02). Conversely, there was no significant difference in median TBR between grade IV (20) and grade III (22.37). These findings support the correlation between high CXCR4 expression, particularly in high-grade gliomas, and elevated uptake of Ga-Pentixafor. While areas with high uptake showed CXCR4 expression, areas with low uptake did not exhibit noticeable expression (data not shown).

CONCLUSION

This study demonstrated that Ga-Cixafor™ PET exhibits a TBR with minimal cortical uptake, significantly enhancing glioma detection compared to conventional imaging methods. This, combined with the potential therapeutic capabilities of CXCR4-targeting radiopharmaceuticals, highlights the promise of Ga-Cixafor™ as a valuable tool for not only improved glioma diagnosis but also personalized treatment strategies.

摘要

背景

虽然磁共振成像(MRI)仍是形态学成像的金标准,但其在细胞水平区分肿瘤组织和治疗引起的变化的能力不足。值得注意的是,胶质瘤细胞,尤其是多形性胶质母细胞瘤(GBM),表现出趋化因子受体4(CXCR4)的过表达。本研究旨在评估非侵入性镓标记的西妥昔单抗(Ga-Cixafor™)PET/CT作为提高高级别胶质瘤患者诊断准确性工具的可行性。

方法

在这项回顾性分析中,利用了一个组织病理学确诊的胶质瘤患者数据库,这些患者的MRI表现与高级别胶质瘤一致。在MRI检查后的2周内,这些患者接受了Ga-Cixafor™ PET/CT扫描以评估CXCR4表达。基于既定标准的视觉评分以及包括最大标准化摄取值(SUV)和肿瘤与本底比值(TBR)在内的半定量测量均被计算出来以分析PET/CT数据。

结果

我们的回顾性研究纳入了29例组织学确诊的胶质瘤患者,其MRI表现与高级别胶质瘤一致。所有患者在MRI检查后的2周内,具体是在注射后1小时的时间点接受了Ga-Cixafor™ PET/CT扫描。基于标准化评分系统的视觉评估在29例扫描中识别出27例阳性扫描(93.1%)。SUV中位数为2.31(范围:0.49 - 9.96),TBR中位数为20(范围:6.12 - 124.5)。病理分析显示29例患者中有5例为III级病变(17.24%)和24例为IV级病变(82.75%)。值得注意的是,IV级病变的SUV中位数(2.85)显著高于III级病变(1.27)(P = 0.02)。相反,IV级病变(20)和III级病变(22.37)的TBR中位数无显著差异。这些发现支持了CXCR4高表达之间的相关性,特别是在高级别胶质瘤中,以及镓标记的西妥昔单抗摄取增加之间的相关性。高摄取区域显示CXCR4表达,而低摄取区域未表现出明显表达(数据未显示)。

结论

本研究表明,Ga-Cixafor™ PET表现出皮质摄取最小的TBR,与传统成像方法相比显著提高了胶质瘤检测。这与靶向CXCR4的放射性药物的潜在治疗能力相结合,突出了Ga-Cixafor™作为不仅用于改善胶质瘤诊断而且用于个性化治疗策略的有价值工具的前景。

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