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Combined iron oxide nanoparticle ferumoxytol and gadolinium contrast enhanced MRI define glioblastoma pseudoprogression

机译:合并氧化铁纳米粒子Ferumoxytol和钆对比增强MRI定义胶质母细胞瘤假冒竞争

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Background Noninvasively differentiating therapy-induced pseudoprogression from recurrent disease in patients with glioblastoma is prospectively difficult due to the current lack of a biologically specific imaging metric. Ferumoxytol iron oxide nanoparticle MRI contrast characterizes innate immunity mediated neuroinflammation; therefore, we hypothesized that combined ferumoxytol and gadolinium enhanced MRI could serve as a biomarker of glioblastoma pseudoprogression.Methods In this institutional review board-approved, retrospective study, we analyzed ferumoxytol and gadolinium contrast enhanced T1-weighted 3T MRI in 45 patients with glioblastoma over multiple clinical timepoints. Isocitrate dehydrogenase 1 (IDH-1) mutational status was characterized by exome sequencing. Sum of products diameter measurements were calculated according to Response Assessment in Neuro-Oncology criteria from both gadolinium and ferumoxytol enhanced sequences. Enhancement mismatch was calculated as the natural log of the ferumoxytol to gadolinium sum of products diameter ratio. Analysis of variance and Student's t-test assessed differences in mismatch ratios. P-value 0.05 indicated statistical significance.Results With the development of pseudoprogression we observed a significantly elevated mismatch ratio compared with disease recurrence (P 0.01) within IDH-1 wild type patients. Patients with IDH-1 mutation demonstrated significantly reduced mismatch ratio with the development of pseudoprogression compared with disease recurrence (P 0.01). Receiver operator curve analysis demonstrated 100% sensitivity and specificity for the use of mismatch ratios as a diagnostic biomarker of pseudoprogression.Conclusion Our study suggests that ferumoxytol to gadolinium contrast mismatch ratios are an MRI biomarker for the diagnosis of pseudoprogression in patients with glioblastoma. This may be due to the unique characterization of therapy-induced neuroinflammation.
机译:背景技术由于目前缺乏生物学特异性的成像度量,未经侵略性地区分治疗诱导的胶质母细胞瘤患者的复发性疾病的假冒竞争。 Ferumoxytol氧化铁纳米粒子MRI对比表征先天免疫介导的神经炎性炎症;因此,我们假设联合的Ferumoxytol和钆增强MRI可以作为胶质母细胞瘤的生物标志物。在这一制度审查委员会审查,回顾性研究中,我们分析了Ferumoxytol和Gadolinium在45名胶质母细胞瘤患者中分析了Ferumoxytol和钆对比度增强的多个临床时间点。异柠檬酸脱氢酶1(IDH-1)突变状态的特征在于exome测序。根据来自钆和Ferumoxytol增强序列的神经诊断标准的响应评估,计算产品总和。增强不匹配是计算为Ferumoxytol的天然原木与钆产物直径比的钆总和。差异和学生的T检验分析分析不匹配比率差异。 P值<0.05表示统计学意义。随着野生型患者的疾病复发(P <0.01),观察到假期竞争的发育明显高的错配比。患有IDH-1突变的患者表现出与疾病复发相比的假冒竞争的发育显着降低(P <0.01)。接收器操作率曲线分析证明了使用不匹配比的100%敏感性和特异性作为假冒波动的诊断生物标志物。结论我们的研究表明,Ferumoxytol对钆对比失控的比率是胶质母细胞瘤患者诊断假冒竞争的MRI生物标志物。这可能是由于治疗诱导的神经炎性炎症的独特表征。

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