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NEURO-IMAGING (CLINICAL AND/OR LABORATORY RESEARCH)

机译:神经影像(临床和/或实验室研究)

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Malignant gliomas include hypoxic cells due to both excessive consumption and insufficient supply of oxygen within the tumor. Intratumoral hypoxic conditions are disadvantageous in term of the production of peroxide radicals, which induces DNA damage under irradiation. Cancer stem cells existing within hypoxic tumor tissue have also been considered to represent a likely cause of radioresistance. In glioblastoma, hypoxic conditions play an important role in the development of tumor progression. Therefore, we performed PET using ~(11)C-methionine for detecting extent of tumor, and using ~(18)F-FRP170 (~(18)F-FRP170 PET) for detecting hypoxic cells in malignant brain tumors. We also examined on ~(18)F-FRP170 PET with intratumoral oxygen pressure (tpO_2 ) within glioblastoma measured using oxygen micro-electrodes during tumor resection. Furthermore, we analyzed hypoxia-related genes, such as HIF-1 and VEGF, in high or low uptake areas of ~(18)F-FRP170 PET. Mean tpO_2 was significantly lower in the high-uptake area than in the low-uptake area. The specimens obtained from high-uptake areas, showed the increased expression of hypoxia-related genes. These findings suggest that high accumulation on ~(18)F-FRP170 PET represents viable hypoxic tissues in glioblastoma.
机译:恶性神经胶质瘤包括低氧细胞,这是由于肿瘤内的氧气消耗过多和氧气供应不足所致。就过氧化物自由基的产生而言,肿瘤内低氧条件是不利的,过氧化物自由基会在辐射下诱导DNA损伤。缺氧肿瘤组织内存在的癌症干细胞也被认为代表了抗辐射的可能原因。在胶质母细胞瘤中,低氧条件在肿瘤进展的发展中起重要作用。因此,我们使用〜(11)C-蛋氨酸检测肿瘤范围,并使用〜(18)F-FRP170(〜(18)F-FRP170 PET)检测恶性脑肿瘤中的低氧细胞。我们还检查了〜(18)F-FRP170 PET,在胶质母细胞瘤中使用了肿瘤切除期间的氧气微电极测量了肿瘤内的氧气压力(tpO_2)。此外,我们分析了〜(18)F-FRP170 PET高或低摄取区域中与缺氧相关的基因,例如HIF-1和VEGF。高摄取区的平均tpO_2明显低于低摄取区。从高摄取区域获得的标本显示缺氧相关基因的表达增加。这些发现表明〜(18)F-FRP170 PET上的高积累代表胶质母细胞瘤中可行的低氧组织。

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    《Neuro-Oncology》 |2014年第5期|v138-v158|共21页
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