首页> 美国卫生研究院文献>Neuro-Oncology >PROGNOSTIC VALUE OF O-(2-18FFLUORETHYL)-L-TYROSINE POSITRON EMISSION TOMOGRAPHY (18FET-PET) WITHIN THE CLINICAL COURSE IN NEWLY DIAGNOSED GLIOBLASTOMA
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PROGNOSTIC VALUE OF O-(2-18FFLUORETHYL)-L-TYROSINE POSITRON EMISSION TOMOGRAPHY (18FET-PET) WITHIN THE CLINICAL COURSE IN NEWLY DIAGNOSED GLIOBLASTOMA

机译:新诊断胶质母细胞瘤临床研究中O-(2- 18F氟基)-L-酪氨酸正电子发射断层显像(18FET-PET)的预后价值

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摘要

BACKGROUND: Aim of this prospective longitudinal study was to identify static and dynamic O-(2-[18F]fluorethyl)-L-tyrosine PET (18FET-PET) derived imaging biomarkers in glioblastoma (GB) patients to obtain additional information concerning prognosis and monitoring of therapy. METHODS: 79 patients with newly diagnosed GB were included; 42 patients underwent stereotactic biopsy (unresectable tumors) and 37 patients microsurgical tumor resection. All patients were scheduled to receive radiotherapy plus concomitant and adjuvant temozolomide (RCx/TMZ). 18FET-PET evaluation using static and dynamic parameters was done prior to biopsy/resection, after resection, 4-6 weeks following RCx and after three cycles of TMZ. Endpoints were survival and progression-free-survival. Prognostic factors were obtained from proportional hazards models. RESULTS: Biological tumor volume before RCx (BTVpreRCx) was the most important 18FET-PET derived imaging biomarker and was independent of MGMT promoter methylation and clinical prognostic factors: patients with smaller BTVpreRCx had significant longer progression free (PFS) and overall survival (OS). 18FET time activity curves (TAC) before treatment and their changes after RCx were also related to outcome: patients with initially increasing TAC and those exhibiting a switch from decreasing to increasing TAC after RCx experienced longer progression-free-survival. CONCLUSIONS: BTVpreRCx and TAC represent important 18FET-PET-derived imaging biomarkers in GB. Increasing TAC are associated with prolonged PFS. The BTVpreRCx is a strong prognostic factor for PFS and OS independent of the mode of surgery. Our data furthermore suggest that patients harbouring resectable GB might benefit from maximal PET-guided tumor resection. SECONDARY CATEGORY: Clinical Neuro-Oncology.
机译:背景:这项前瞻性纵向研究的目的是鉴定胶质母细胞瘤(GB)患者中的静态和动态O-(2- [18F]氟乙基)-L-酪氨酸PET(18FET-PET)衍生的成像生物标记物,以获得有关预后和监测治疗。方法:纳入79例新诊断为GB的患者。 42例患者接受了立体定位活检(无法切除的肿瘤),37例接受了显微外科手术切除。所有患者均计划接受放疗,以及伴随和辅助的替莫唑胺(RCx / TMZ)。在活检/切除之前,切除之后,RCx后4-6周和TMZ的三个周期后,使用静态和动态参数进行18FET-PET评估。终点是生存期和无进展生存期。从比例风险模型中获得预后因素。结果:RCx前的生物肿瘤体积(BTVpreRCx)是最重要的18FET-PET衍生成像生物标志物,并且与MGMT启动子甲基化和临床预后因素无关:BTVpreRCx较小的患者的无进展生存期(PFS)和总体生存期(OS)明显更长。治疗前的18FET时间活动曲线(TAC)及其在RCx后的变化也与结局有关:最初TAC升高的患者以及RCx后表现出从TAC降低到升高TAC的患者经历了更长的无进展生存期。结论:BTVpreRCx和TAC代表GB中重要的18FET-PET衍生成像生物标记。 TAC增加与PFS延长有关。 BTVpreRCx是独立于手术方式的PFS和OS的强大预后因素。我们的数据进一步表明,具有可切除GB的患者可能会从最大的PET引导的肿瘤切除术中受益。第二类:临床神经肿瘤学。

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