Pathophysiological aspects of malignant brain tumors studied with positron emission tomography.

J O Jarden
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Abstract

To further understand the control of brain tumor fluid balance and pH, the following studies were undertaken. The transport of a water soluble molecule across the brain and tumor capillary endothelium was studied during glucocorticoid and radiation treatment. The brain and brain-tumor acidity (pH) was evaluated as a single measurement in patients receiving a low maintenance dose of glucocorticoid. Transport changes and pH were measured in 61 patients with cerebral tumors using 82Rubidium (82Rb) and 11C-Dimethyloxa-zolidindione (11C-DMO), respectively, and Positron Emission Tomography (PET). Supplementary studies of tumor and contralateral brain blood flow and blood volume using the C15O2/PET and C15O/PET technique, respectively, were included to validate the 82Rb/PET model and obtain further information. A total of 125 PET scans were performed. Supplementary studies were undertaken to estimate delay of blood registration and form distribution of arterial blood isotope activity curves. Blood-to-tumor barrier transport was outlined at baseline and at 6 and 24 hours after the start of glucocorticoid treatment, finding a significant decrease in the transport. Radiation treatment (2-6 gray) did not alter the blood-to-tumor barrier transport when restudied within one hour in patients receiving glucocorticoid. In accordance with others, we observed pH values in gray and white matter in the range of 6.74-7.09 and 6.77-7.03 respectively. The pH in brain tumors was as high as 6.88-7.26, suggesting that tumors are more alkalotic than the normal brain. The permeability surface area product and the permeability coefficient were determined from the 82Rb/PET transport and C15O2/PET flow studies. Baseline permeability values were comparable to the literature values both for 82Rb and potassium. No difference in tissue blood volume was seen between 82Rb/PET and C15O/PET models and was of the same magnitude in the tumor and the contralateral tissue. The pH and fluid control in human brain tumors are perceived as metabolically controlled rather than, as previously believed, a result of simple passive exchange of alkalotic or osmotic active molecules between plasma and tumor interstitial space. Aspects of tumor alkalosis, tumor edema production, glucocorticoid edema clearance, and relationship between the anti-edema effect of glucocorticoid and the shown transport changes to 82Rb will be reviewed in the light of metabolic control mechanisms.

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用正电子发射断层扫描研究恶性脑肿瘤的病理生理方面。
为了进一步了解脑肿瘤体液平衡和pH值的控制,进行了以下研究。在糖皮质激素和放射治疗期间,研究了一种水溶性分子在脑和肿瘤毛细血管内皮中的运输。在接受低维持剂量糖皮质激素的患者中,脑和脑肿瘤酸度(pH)作为单一测量进行评估。采用82铷(82Rb)和11c -二甲氧嘧啶-唑啶酮(11C-DMO)及正电子发射断层扫描(PET)检测61例脑肿瘤患者的转运变化和pH。分别采用C15O2/PET和C15O/PET技术对肿瘤和对侧脑血流量和血容量进行补充研究,以验证82Rb/PET模型并获得进一步信息。共进行125次PET扫描。还进行了补充研究,以估计血液登记的延迟和动脉血同位素活性曲线的分布。在基线和糖皮质激素治疗开始后的6小时和24小时,血液到肿瘤屏障的运输被概述,发现运输显著减少。当接受糖皮质激素治疗的患者在1小时内重新研究时,放射治疗(2-6灰色)没有改变血液到肿瘤屏障的运输。根据其他人,我们观察到灰质和白质的pH值分别在6.74-7.09和6.77-7.03之间。脑肿瘤的pH值高达6.88-7.26,表明肿瘤比正常大脑具有更强的碱碱性。通过82Rb/PET输运和C15O2/PET流动研究确定了渗透表面积积和渗透系数。基线渗透率值与82Rb和钾的文献值相当。82Rb/PET模型与C15O/PET模型的组织血容量无差异,肿瘤与对侧组织的血容量大小相同。人脑肿瘤中的pH值和体液控制被认为是由代谢控制的,而不是像以前认为的那样,是血浆和肿瘤间质间隙之间碱性或渗透性活性分子简单被动交换的结果。本文将结合代谢调控机制,对肿瘤碱中毒、肿瘤水肿产生、糖皮质激素水肿清除、糖皮质激素抗水肿作用与82Rb转运变化的关系等方面进行综述。
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Proceedings of the Annual Meeting of the Norwegian Neurological Association. November 2010. Oslo, Norway. Selected articles from the Annual Meeting of the Norwegian Neurological Association, November 2009, Oslo, Norway. Selected articles from the Annual Meeting of the Norwegian Neurological Association, 26-30 November 2007, Oslo, Norway. Advances in the pathophysiology of status epilepticus. Childhood convulsive status epilepticus: epidemiology, management and outcome.
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