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在原位移植人源胶质母细胞瘤细胞系的大鼠模型中,通过多参数 MRI 和 MRS 对与异柠檬酸脱氢酶 1 突变表达相关的生理和代谢变化进行体内特征分析。

In vivo characterization of physiological and metabolic changes related to isocitrate dehydrogenase 1 mutation expcression by multiparametric MRI and MRS in a rat model with orthotopically grafted human-derived glioblastoma cell lines.

机构信息

Nancyclotep Molecular and Experimental Imaging Platform, CHRU Nancy, Nancy, France.

Lorraine University, INSERM, IADI UMR 1254, Nancy, France.

出版信息

NMR Biomed. 2021 Jun;34(6):e4490. doi: 10.1002/nbm.4490. Epub 2021 Feb 17.

DOI:10.1002/nbm.4490
PMID:33599048
Abstract

The physiological mechanism induced by the isocitrate dehydrogenase 1 (IDH1) mutation, associated with better treatment response in gliomas, remains unknown. The aim of this preclinical study was to characterize the IDH1 mutation through in vivo multiparametric MRI and MRS. Multiparametric MRI, including the measurement of blood flow, vascularity, oxygenation, permeability, and in vivo MRS, was performed on a 4.7 T animal MRI system in rat brains grafted with human-derived glioblastoma U87 cell lines expressing or not the IDH1 mutation by the CRISPR/Cas9 method, and secondarily characterized with additional ex vivo HR-MAS and histological analyses. In univariate analyses, compared with IDH1-, IDH1+ tumors exhibited higher vascular density (p < 0.01) and better perfusion (p = 0.02 for cerebral blood flow), but lower vessel permeability (p < 0.01 for time to peak (TTP), p = 0.04 for contrast enhancement) and decreased T map values (p = 0.02). Using linear discriminant analysis, vascular density and TTP values were found to be independent MRI parameters for characterizing the IDH1 mutation (p < 0.01). In vivo MRS and ex vivo HR-MAS analysis showed lower metabolites of tumor aggressiveness for IDH1+ tumors (p < 0.01). Overall, the IDH1 mutation exhibited a higher vascularity on MRI, a lower permeability, and a less aggressive metabolic profile. These MRI features may prove helpful to better pinpoint the physiological mechanisms induced by this mutation.

摘要

IDH1 突变诱导的生理机制与脑胶质瘤的更好治疗反应相关,但具体机制尚不清楚。本临床前研究旨在通过体内多参数 MRI 和 MRS 对 IDH1 突变进行特征描述。在 4.7T 动物 MRI 系统上对大鼠脑进行多参数 MRI 检查,包括血流、血管性、氧合、通透性的测量以及体内 MRS,该系统使用 CRISPR/Cas9 方法将表达或不表达 IDH1 突变的人源胶质母细胞瘤 U87 细胞系移植到大鼠脑内,随后进行额外的 HR-MAS 和组织学分析。在单变量分析中,与 IDH1-肿瘤相比,IDH1+肿瘤具有更高的血管密度(p < 0.01)和更好的灌注(p = 0.02 用于脑血流),但更低的血管通透性(p < 0.01 用于达峰时间(TTP),p = 0.04 用于对比增强)和 T 映射值降低(p = 0.02)。使用线性判别分析发现,血管密度和 TTP 值是用于特征描述 IDH1 突变的独立 MRI 参数(p < 0.01)。体内 MRS 和体外 HR-MAS 分析显示 IDH1+肿瘤的侵袭性代谢物较低(p < 0.01)。总体而言,IDH1 突变在 MRI 上表现出更高的血管密度、更低的通透性和侵袭性较低的代谢特征。这些 MRI 特征可能有助于更好地确定该突变诱导的生理机制。

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