首页> 美国卫生研究院文献>Neuro-oncology Advances >OTHR-14. TREATMENT MONITORING OF IMMUNOTHERAPY AND TARGETED THERAPY USING FET PET IN PATIENTS WITH MELANOMA AND LUNG CANCER BRAIN METASTASES: INITIAL EXPERIENCES
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OTHR-14. TREATMENT MONITORING OF IMMUNOTHERAPY AND TARGETED THERAPY USING FET PET IN PATIENTS WITH MELANOMA AND LUNG CANCER BRAIN METASTASES: INITIAL EXPERIENCES

机译:OTHR-14。 FET PET治疗黑色素瘤和肺癌脑转移的患者的免疫疗法的治疗监测和靶向治疗:初步经验

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摘要

BACKGROUND: Due to the lack of specificity of contrast-enhanced (CE) MRI, both the response assessment and differentiation of progression from pseudoprogression (PsP) following immunotherapy using checkpoint inhibitors (ICI) or targeted therapy (TT) may be challenging, especially when ICI or TT is applied in combination with radiotherapy (RT). Here, we evaluated the value of amino acid PET using O-(2-[ F]fluoroethyl)-L-tyrosine (FET) as a problem-solving tool in comparison to CE-MRI in patients with brain metastases (BM) secondary to malignant melanoma (MM) and NSCLC. METHODS: We retrospectively identified 31 patients with 74 BM secondary to MM (n=20 with 42 BM) and NSCLC (n=11 with 32 BM) who underwent 52 FET-PET scans during the course of disease. All patients had RT prior to ICI or TT initiation (61%) or RT concurrent to ICI or TT (39%). In 13 patients, FET-PET was performed for treatment response assessment of ICI or TT using baseline and follow-up scans (median time between scans, 4.2 months). In the remaining 18 patients, FET-PET was used for the differentiation of progression from PsP related to RT plus ICI or TT. In all BM, metabolic activity on FET-PET was evaluated by calculation of tumor/brain ratios. FET-PET imaging findings were compared to CE-MRI and correlated to the clinical follow-up or neuropathological findings after neuroimaging. RESULTS: In 4 of 13 patients (31%), FET-PET provided additional information for treatment response evaluation beyond the information provided by CE-MRI alone. Furthermore, responding patients on FET-PET had a median stable clinical follow-up of 10 months. In 10 of 18 patients (56%) with CE-MRI findings suggesting progression, FET-PET detected PsP. In 9 of these 10 patients, PsP was confirmed by a median stable clinical follow-up of 11 months. CONCLUSIONS: FET-PET may add valuable information for treatment monitoring in individual BM patients undergoing RT in combination with ICI or TT.
机译:背景:由于缺乏增强造影(CE)MRI的特异性,在使用检查点抑制剂(ICI)或靶向治疗(TT)进行免疫治疗后,反应评估和从伪进展(PsP)的进展分化可能都具有挑战性,特别是在ICI或TT与放疗(RT)结合使用。在这里,我们评估了使用O-(2- [F]氟乙基)-L-酪氨酸(FET)作为与CE-MRI相比可解决继发于脑转移(BM)的患者的问题解决工具的氨基酸PET的价值恶性黑色素瘤(MM)和非小细胞肺癌。方法:我们回顾性分析了31例继发于MM的74 BM的患者(n = 20 = 42 BM)和NSCLC(n = 11 = 32 BM)在病程中进行了52次FET-PET扫描。所有患者均在ICI或TT发作之前进行RT(61%),或在ICI或TT并发之前进行RT(39%)。在13例患者中,使用基线和随访扫描(两次扫描之间的中位时间为4.2个月)进行FET-PET,以评估ICI或TT的治疗反应。在其余18例患者中,使用FET-PET来区分与RT加ICI或TT相关的PsP进展。在所有BM中,通过计算肿瘤/脑比来评估对FET-PET的代谢活性。 FET-PET影像学检查结果与CE-MRI进行比较,并与神经影像学检查后的临床随访或神经病理学检查结果相关。结果:在13例患者中有4例(31%)中,FET-PET提供了单独CE-MRI所提供信息之外的其他治疗反应评估信息。此外,接受FET-PET治疗的患者中位稳定的临床随访时间为10个月。在18例CE-MRI表现提示进展的患者中(10%),FET-PET检测到PsP。在这10例患者中的9例中,通过中位11个月的稳定临床随访证实了PsP。结论:FET-PET可能为接受RT结合ICI或TT的BM个体患者的治疗监测提供有价值的信息。

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