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通过正电子发射断层扫描测量的甲基-[11C]-L-蛋氨酸摄取与胶质瘤患者的微血管密度相关。

Methyl-[11C]- l-methionine uptake as measured by positron emission tomography correlates to microvessel density in patients with glioma.

作者信息

Kracht Lutz W, Friese Michael, Herholz Karl, Schroeder Roland, Bauer Bernd, Jacobs Andreas, Heiss Wolf-Dieter

机构信息

Max-Planck-Institut für neurologische Forschung, Cologne, Germany.

出版信息

Eur J Nucl Med Mol Imaging. 2003 Jun;30(6):868-73. doi: 10.1007/s00259-003-1148-7. Epub 2003 Apr 12.

Abstract

Positron emission tomography (PET) using methyl-[(11)C]- l-methionine ([(11)C]MET) is a useful tool in the diagnosis of brain tumours. The main mechanism of [(11)C]MET uptake is probably increased transport via the L-transporter system located in the endothelial cell membrane. We used [(11)C]MET-PET and microvessel count in glioma specimens to investigate whether the increased amino acid uptake is related to angiogenesis. Twenty-one patients with newly diagnosed and histologically confirmed glioma were investigated with [(11)C]MET-PET before open surgery. [(11)C]MET uptake was determined within an 8-mm region of interest in the area of the tumour showing the highest uptake, and the ratio to uptake in the corresponding contralateral region was calculated. To measure angiogenesis, immunostaining with factor VIII antibody was applied to sections from tumour tissue, and highlighted microvessels were counted in the area of highest vascularisation. In the entire patient group, a positive correlation was found between microvessel count and [(11)C]MET uptake (Spearman: r=0.89, P<0.001). This correlation was also significant in subgroups of patients [patients with grade II and III astrocytomas (Spearman: r=0.77, P<0.01) and patients with glioblastoma (Spearman: r=0.64, P<0.05)]. Angiogenesis, as assessed by microvessel count, and increased amino acid uptake, as assessed by [(11)C]MET-PET, are closely related events in gliomas. [(11)C]MET-PET offers a direct measure of amino acid transport and an indirect measure of microvessel density. [(11)C]MET-PET might be a useful tool to select potential responders to anti-angiogenic therapy and to monitor patients during such therapy.

摘要

使用甲基-[(11)C]-L-蛋氨酸([(11)C]MET)的正电子发射断层扫描(PET)是诊断脑肿瘤的一种有用工具。[(11)C]MET摄取的主要机制可能是通过位于内皮细胞膜的L转运系统的转运增加。我们使用[(11)C]MET-PET和胶质瘤标本中的微血管计数来研究氨基酸摄取增加是否与血管生成有关。21例新诊断并经组织学证实的胶质瘤患者在开颅手术前行[(11)C]MET-PET检查。在肿瘤摄取最高区域的8毫米感兴趣区内测定[(11)C]MET摄取,并计算与相应对侧区域摄取的比值。为了测量血管生成,将因子VIII抗体免疫染色应用于肿瘤组织切片,并在血管化最高的区域计数突出显示的微血管。在整个患者组中,微血管计数与[(11)C]MET摄取之间存在正相关(Spearman:r=0.89,P<0.001)。这种相关性在患者亚组中也很显著[II级和III级星形细胞瘤患者(Spearman:r=0.77,P<0.01)和胶质母细胞瘤患者(Spearman:r=0.64,P<0.05)]。通过微血管计数评估的血管生成和通过[(11)C]MET-PET评估的氨基酸摄取增加是胶质瘤中密切相关的事件。[(11)C]MET-PET提供了氨基酸转运的直接测量和微血管密度的间接测量。[(11)C]MET-PET可能是选择抗血管生成治疗潜在反应者以及在此类治疗期间监测患者的有用工具。

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