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脑肿瘤中的18F - 多巴动力学

18F-FDOPA kinetics in brain tumors.

作者信息

Schiepers Christiaan, Chen Wei, Cloughesy Timothy, Dahlbom Magnus, Huang Sung-Cheng

机构信息

Department of Molecular and Medical Pharmacology, David Geffen School of Medicine, University of California, Los Angeles, California, USA.

出版信息

J Nucl Med. 2007 Oct;48(10):1651-61. doi: 10.2967/jnumed.106.039321. Epub 2007 Sep 14.

Abstract

UNLABELLED

L-3,4-Dihydroxy-6-(18)F-fluoro-phenyl-alanine ((18)F-FDOPA) is an amino acid analog used to evaluate presynaptic dopaminergic neuronal function. Evaluation of tumor recurrence in neurooncology is another application. Here, the kinetics of (18)F-FDOPA in brain tumors were investigated.

METHODS

A total of 37 patients underwent 45 studies; 10 had grade IV, 10 had grade III, and 13 had grade II brain tumors; 2 had metastases; and 2 had benign lesions. After (18)F-DOPA was administered at 1.5-5 MBq/kg, dynamic PET images were acquired for 75 min. Images were reconstructed with iterative algorithms, and corrections for attenuation and scatter were applied. Images representing venous structures, the striatum, and tumors were generated with factor analysis, and from these, input and output functions were derived with simple threshold techniques. Compartmental modeling was applied to estimate rate constants.

RESULTS

A 2-compartment model was able to describe (18)F-FDOPA kinetics in tumors and the cerebellum but not the striatum. A 3-compartment model with corrections for tissue blood volume, metabolites, and partial volume appeared to be superior for describing (18)F-FDOPA kinetics in tumors and the striatum. A significant correlation was found between influx rate constant K and late uptake (standardized uptake value from 65 to 75 min), whereas the correlation of K with early uptake was weak. High-grade tumors had significantly higher transport rate constant k(1), equilibrium distribution volumes, and influx rate constant K than did low-grade tumors (P < 0.01). Tumor uptake showed a maximum at about 15 min, whereas the striatum typically showed a plateau-shaped curve. Patlak graphical analysis did not provide accurate parameter estimates. Logan graphical analysis yielded reliable estimates of the distribution volume and could separate newly diagnosed high-grade tumors from low-grade tumors.

CONCLUSION

A 2-compartment model was able to describe (18)F-FDOPA kinetics in tumors in a first approximation. A 3-compartment model with corrections for metabolites and partial volume could adequately describe (18)F-FDOPA kinetics in tumors, the striatum, and the cerebellum. This model suggests that (18)F-FDOPA was transported but not trapped in tumors, unlike in the striatum. The shape of the uptake curve appeared to be related to tumor grade. After an early maximum, high-grade tumors had a steep descending branch, whereas low-grade tumors had a slowly declining curve, like that for the cerebellum but on a higher scale.

摘要

未标注

L-3,4-二羟基-6-(18)F-氟苯丙氨酸((18)F-FDOPA)是一种用于评估突触前多巴胺能神经元功能的氨基酸类似物。评估神经肿瘤学中的肿瘤复发是其另一应用。在此,对(18)F-FDOPA在脑肿瘤中的动力学进行了研究。

方法

共37例患者接受了45项研究;其中10例为IV级脑肿瘤,10例为III级,13例为II级脑肿瘤;2例有转移瘤;2例有良性病变。以1.5 - 5 MBq/kg的剂量给予(18)F-DOPA后,采集75分钟的动态PET图像。图像用迭代算法重建,并进行衰减和散射校正。通过因子分析生成代表静脉结构、纹状体和肿瘤的图像,并利用简单阈值技术从中导出输入和输出函数。应用房室模型估计速率常数。

结果

二房室模型能够描述(18)F-FDOPA在肿瘤和小脑中的动力学,但不能描述在纹状体中的动力学。一个对组织血容量、代谢物和部分容积进行校正的三房室模型似乎在描述(18)F-FDOPA在肿瘤和纹状体中的动力学方面更具优势。流入速率常数K与晚期摄取(65至75分钟的标准化摄取值)之间存在显著相关性,而K与早期摄取的相关性较弱。高级别肿瘤的转运速率常数k(1)、平衡分布容积和流入速率常数K显著高于低级别肿瘤(P < 0.01)。肿瘤摄取在约15分钟时达到最大值,而纹状体通常呈现平台形曲线。Patlak图形分析未提供准确的参数估计。Logan图形分析得出了可靠的分布容积估计值,并能区分新诊断的高级别肿瘤和低级别肿瘤。

结论

二房室模型能够初步描述(18)F-FDOPA在肿瘤中的动力学。一个对代谢物和部分容积进行校正的三房室模型能够充分描述(18)F-FDOPA在肿瘤、纹状体和小脑中的动力学。该模型表明,与纹状体不同,(18)F-FDOPA在肿瘤中被转运但未被滞留。摄取曲线的形状似乎与肿瘤级别有关。在早期达到最大值后,高级别肿瘤有一个陡峭的下降分支,而低级别肿瘤有一个缓慢下降的曲线,类似于小脑但幅度更高。

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