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Mesoscopic imaging of glioblastomas: Are diffusion perfusion and spectroscopic measures influenced by the radiogenetic phenotype?

机译:胶质母细胞瘤的介观成像:扩散灌注和光谱学方法是否受放射遗传表型影响?

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摘要

The purpose of this study was to identify markers from perfusion, diffusion, and chemical shift imaging in glioblastomas (GBMs) and to correlate them with genetically determined and previously published patterns of structural magnetic resonance (MR) imaging. Twenty-six patients (mean age 60 years, 13 female) with GBM were investigated. Imaging consisted of native and contrast-enhanced 3D data, perfusion, diffusion, and spectroscopic imaging. In the presence of minor necrosis, cerebral blood volume (CBV) was higher (median ± SD, 2.23% ± 0.93) than in pronounced necrosis (1.02% ± 0.71), pcorr = 0.0003. CBV adjacent to peritumoral fluid-attenuated inversion recovery (FLAIR) hyperintensity was lower in edema (1.72% ± 0.31) than in infiltration (1.91% ± 0.35), pcorr = 0.039. Axial diffusivity adjacent to peritumoral FLAIR hyperintensity was lower in severe mass effect (1.08*10–3 mm2/s ± 0.08) than in mild mass effect (1.14*10–3 mm2/s ± 0.06), pcorr = 0.048. Myo-inositol was positively correlated with a marker for mitosis (Ki-67) in contrast-enhancing tumor, r = 0.5, pcorr = 0.0002. Changed CBV and axial diffusivity, even outside FLAIR hyperintensity, in adjacent normal-appearing matter can be discussed as to be related to angiogenesis pathways and to activated proliferation genes. The correlation between myo-inositol and Ki-67 might be attributed to its binding to cell surface receptors regulating tumorous proliferation of astrocytic cells.
机译:这项研究的目的是从胶质母细胞瘤(GBM)的灌注,扩散和化学位移成像中鉴定标记物,并将其与遗传学确定的和先前发表的结构磁共振(MR)成像模式相关联。调查了26例GBM患者(平均年龄60岁,女性13岁)。成像由原始的和对比度增强的3D数据,灌注,扩散和光谱成像组成。在轻微坏死的情况下,脑血容量(CBV)高于明显坏死(1.02%±0.71),中位数±SD,2.23%±0.93,pcorr = 0.0003。与瘤周液减低反转恢复(FLAIR)高强度相邻的CBV在水肿(1.72%±0.31)低于在浸润(1.91%±0.35),pcorr = 0.039。严重肿块效应(1.08 * 10 –3 mm 2 / s±0.08)与瘤周FLAIR高强度相邻的轴扩散性低于轻度肿块效应(1.14 * 10 < sup> –3 mm 2 / s±0.06),pcorr = 0.048。肌醇与造影剂增强肿瘤中的有丝分裂标记(Ki-67)呈正相关,r = 0.5,pcorr = 0.0002。甚至在邻近正常出现的物质中,即使在FLAIR高强度之外,CBV和轴向扩散率的变化也可以讨论为与血管生成途径和激活的增殖基因有关。肌醇和Ki-67之间的相关性可能归因于其与调节星形胶质细胞肿瘤增殖的细胞表面受体的结合。

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