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在体 MRS 测量 IDH 突变型异种移植小鼠模型与脑肿瘤患者中 2-羟戊二酸的含量。

In vivo MRS measurement of 2-hydroxyglutarate in patient-derived IDH-mutant xenograft mouse models versus glioma patients.

机构信息

Advanced Imaging Research Center, University of Texas Southwestern Medical Center, Dallas, Texas.

Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas.

出版信息

Magn Reson Med. 2020 Sep;84(3):1152-1160. doi: 10.1002/mrm.28183. Epub 2020 Jan 30.

Abstract

PURPOSE

To generate a preclinical model of isocitrate dehydrogenase (IDH) mutant gliomas from glioma patients and design a MRS method to test the compatibility of 2-hydroxyglutarate (2HG) production between the preclinical model and patients.

METHODS

Five patient-derived xenograft (PDX) mice were generated from two glioma patients with IDH1 R132H mutation. A PRESS sequence was tailored at 9.4 T, with computer simulation and phantom analyses, for improving 2HG detection in mice. 2HG and other metabolites in the PDX mice were measured using the optimized MRS at 9.4 T and compared with 3 T MRS measurements of the metabolites in the parental-tumor patients. Spectral fitting was performed with LCModel using in-house basis spectra. Metabolite levels were quantified with reference to water.

RESULTS

The PRESS TE was optimized to be 96 ms, at which the 2HG 2.25 ppm signal was narrow and inverted, thereby leading to unequivocal separation of the 2HG resonance from adjacent signals from other metabolites. The optimized MRS provided precise detection of 2HG in mice compared to short-TE MRS at 9.4 T. The 2HG estimates in PDX mice were in excellent agreement with the 2HG measurements in the patients.

CONCLUSION

The similarity of 2HG production between PDX models and parental-tumor patients indicates that PDX tumors retain the parental IDH metabolic fingerprint and can serve as a preclinical model for improving our understanding of the IDH-mutation associated metabolic reprogramming.

摘要

目的

从胶质瘤患者中生成异柠檬酸脱氢酶(IDH)突变型神经胶质瘤的临床前模型,并设计 MRS 方法来测试临床前模型和患者之间 2-羟戊二酸(2HG)生成的兼容性。

方法

从两名 IDH1 R132H 突变的胶质瘤患者中生成了 5 名患者来源的异种移植(PDX)小鼠。针对 9.4T 设计了 PRESS 序列,通过计算机模拟和体模分析,提高了小鼠中 2HG 的检测能力。使用优化的 9.4T MRS 测量 PDX 小鼠中的 2HG 和其他代谢物,并与母肿瘤患者的代谢物的 3T MRS 测量值进行比较。使用 LCModel 进行谱拟合,使用内部基础谱。代谢物水平用水定量。

结果

优化了 PRESS TE 为 96ms,此时 2HG 2.25ppm 信号变窄并反转,从而使 2HG 共振与来自其他代谢物的相邻信号的分离变得明确。与 9.4T 的短 TE MRS 相比,优化的 MRS 能够更精确地检测小鼠中的 2HG。PDX 小鼠中的 2HG 估计与患者中的 2HG 测量值非常吻合。

结论

PDX 模型和母肿瘤患者之间 2HG 生成的相似性表明,PDX 肿瘤保留了母代 IDH 代谢指纹,可作为临床前模型,用于提高我们对 IDH 突变相关代谢重编程的理解。

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