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首页> 外文期刊>European Journal of Nuclear Medicine and Molecular Imaging >Imaging glioma biology: spatial comparison of amino acid PET, amide proton transfer, and perfusion-weighted MRI in newly diagnosed gliomas
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Imaging glioma biology: spatial comparison of amino acid PET, amide proton transfer, and perfusion-weighted MRI in newly diagnosed gliomas

机译:成像神经胶质瘤生物学:新诊断的胶质瘤中氨基酸PET,酰胺质子转移和灌注加权MRI的空间比较

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Purpose Imaging glioma biology holds great promise to unravel the complex nature of these tumors. Besides well-established imaging techniques such O-(2-[18F]fluoroethyl)-l-tyrosine (FET)-PET and dynamic susceptibility contrast (DSC) perfusion imaging, amide proton transfer-weighted (APTw) imaging has emerged as a promising novel MR technique. In this study, we aimed to better understand the relation between these imaging biomarkers and how well they capture cellularity and vascularity in newly diagnosed gliomas. Methods Preoperative MRI and FET-PET data of 46 patients (31 glioblastoma and 15 lower-grade glioma) were segmented into contrast-enhancing and FLAIR-hyperintense areas. Using established cutoffs, we calculated hot-spot volumes (HSV) and their spatial overlap. We further investigated APTw and CBV values in FET-HSV. In a subset of 10 glioblastoma patients, we compared cellularity and vascularization in 34 stereotactically targeted biopsies with imaging. Results In glioblastomas, the largest HSV was found for APTw, followed by PET and CBV (p < 0.05). In lower-grade gliomas, APTw-HSV was clearly lower than in glioblastomas. The spatial overlap of HSV was highest between APTw and FET in both tumor entities and regions. APTw correlated significantly with cellularity, similar to FET, while the association with vascularity was more pronounced in CBV and FET. Conclusions We found a relevant spatial overlap in glioblastomas between hotspots of APTw and FET both in contrast-enhancing and FLAIR-hyperintense tumor. As suggested by earlier studies, APTw was lower in lower-grade gliomas compared with glioblastomas. APTw meaningfully contributes to biological imaging of gliomas.
机译:目的成像神经胶质瘤生物学具有很大的承诺,以解析这些肿瘤的复杂性质。除了良好成熟的成像技术外,这种O-(2- [18F]氟乙基)-1-酪氨酸(FET)-PPET和动态敏感性对比(DSC)灌注成像,酰胺质子转移加权(APTW)成像已成为有希望的新的MR技术。在这项研究中,我们旨在更好地了解这些成像生物标志物之间的关系以及它们在新诊断的胶质瘤中捕获细胞性和血管性的关系。方法术前MRI和46名患者(31种胶质母细胞瘤和15级胶质瘤)的FET-PET数据被分段为对比增强和展实过敏区域。使用已建立的截止值,我们计算了热点卷(HSV)及其空间重叠。我们进一步调查了FET-HSV中的APTW和CBV值。在10个胶质母细胞瘤患者的亚空间中,我们在34种立体定向靶向活组织检查中比较了细胞性和血管化。结果在Glioblastomas,发现最大的HSV用于APTW,其次是PET和CBV(P <0.05)。在较低级的胶质瘤中,APTW-HSV显然低于Glioblastomas。 HSV的空间重叠在肿瘤实体和地区的APTW和FET之间是最高的。 Aptw与细胞性显着相关,类似于FET,而与血管性的关联在CBV和FET中更加明显。结论我们在对比增强和摇摆过度肿瘤中发现了APTW和FET的热点之间的Glioblastomas中的相关空间重叠。如早期研究所述,与Glioblastomas相比,较低级Gliomas的APTW较低。 APTW有意义地有助于Gliomas的生物成像。

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