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通过磁共振成像/磁共振波谱对实验性乳腺癌细胞脑转移小鼠模型进行初步表征。

Preliminary characterization of an experimental breast cancer cells brain metastasis mouse model by MRI/MRS.

作者信息

Simões R V, Martinez-Aranda A, Martín B, Cerdán S, Sierra A, Arús C

机构信息

Grup d'Aplicacions Biomèdiques de la Ressonància Magnètica Nuclear , Universitat Autònoma de Barcelona, Cerdanyola del Vallès, Spain.

出版信息

MAGMA. 2008 Jul;21(4):237-49. doi: 10.1007/s10334-008-0114-6. Epub 2008 May 31.

Abstract

PURPOSE

Chemotherapy increases survival in breast cancer patients. Consequently, cerebral metastases have recently become a significant clinical problem, with an incidence of 30-40% among breast carcinoma patients. As this phenomenon cannot be studied longitudinally in humans, models which mimic brain metastasis are needed to investigate its pathogenesis. Such models may later be used in experimental therapeutic approaches.

MATERIAL AND METHODS/RESULTS: We report a model in which 69% of the animals (9/13 BALB/c nude mice) developed MR-detectable abnormal masses in the brain parenchyma within a 20 to 62-day time window post intra-carotid injection of 435-Br1 human cells. The masses detected in vivo were either single (7 animals) or multiple (2 animals). Longitudinal MR (MRI/MRS) studies and post-mortem histological data were correlated, revealing a total incidence of experimental brain metastases of 85% in the cases studied (11/13 animals). ADC maps perfectly differentiated edema and/or CSF areas from metastasis. Preliminary MRS data also revealed additional features: decrease in N-acetyl aspartate (NAA) was the first MRS-based marker of metastasis growth in the brain (micrometastasis); choline-containing compounds (Cho) rose and creatine (Cr) levels decreased as these lesions evolved, with mobile lipids and lactate also becoming visible. Furthermore, MRS pattern recognition-based analysis suggested that this approach may help to discriminate different growth stages.

CONCLUSIONS

This study paves the way for further in vivo studies oriented towards detection of different tumor progression states and for improving treatment efficiency.

摘要

目的

化疗可提高乳腺癌患者的生存率。因此,脑转移最近已成为一个重大的临床问题,在乳腺癌患者中的发生率为30%-40%。由于无法在人体中对这一现象进行纵向研究,因此需要建立模拟脑转移的模型来研究其发病机制。此类模型随后可用于实验性治疗方法。

材料与方法/结果:我们报告了一种模型,在经颈动脉注射435-Br1人细胞后的20至62天时间窗内,69%的动物(9/13只BALB/c裸鼠)在脑实质内出现了磁共振成像(MR)可检测到的异常肿块。体内检测到的肿块为单个(7只动物)或多个(2只动物)。纵向MR(MRI/MRS)研究与死后组织学数据相关联,在所研究的病例中(11/13只动物),实验性脑转移的总发生率为85%。表观扩散系数(ADC)图能够完美地区分水肿和/或脑脊液区域与转移灶。初步的磁共振波谱(MRS)数据还揭示了其他特征:N-乙酰天门冬氨酸(NAA)降低是脑内转移灶生长(微转移)的首个基于MRS的标志物;随着这些病变的发展,含胆碱化合物(Cho)升高而肌酸(Cr)水平降低,同时可观察到移动脂质和乳酸。此外,基于MRS模式识别的分析表明,这种方法可能有助于区分不同的生长阶段。

结论

本研究为进一步开展旨在检测不同肿瘤进展状态及提高治疗效率的体内研究铺平了道路。

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