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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Magnetic resonance imaging-based detection of glial brain tumors in mice after antiangiogenic treatment.
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Magnetic resonance imaging-based detection of glial brain tumors in mice after antiangiogenic treatment.

机译:抗血管生成治疗后基于磁共振成像的小鼠胶质细胞脑瘤检测。

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Proper delineation of gliomas using contrast-enhanced magnetic resonance imaging (CE-MRI) poses a problem in neuro-oncology. The blood brain barrier (BBB) in areas of diffuse-infiltrative growth may be intact, precluding extravasation and subsequent MR-based detection of the contrast agent gadolinium diethylenetriaminepenta-acetic acid (Gd-DTPA). Treatment with antiangiogenic compounds may further complicate tumor detection as such compounds can restore the BBB in angiogenic regions. The increasing number of clinical trials with antiangiogenic compounds for treatment of gliomas calls for the development of alternative imaging modalities. Here we investigated whether CE-MRI using ultrasmall particles of iron oxide (USPIO, Sinerem) as blood pool contrast agent has additional value for detection of glioma in the brain of nude mice. We compared conventional T1-weighted Gd-DTPA-enhanced MRI to T2*-weighted USPIO-enhanced MRI in mice carrying orthotopic U87 glioma, which were either or not treated with the antiangiogenic compound vandetanib (ZD6474, ZACTIMA). In untreated animals, vessel leakage within the tumor and a relatively high tumor blood volume resulted in good MRI visibility with Gd-DTPA- and USPIO-enhanced MRI, respectively. Consistent with previous findings, vandetanib treatment restored the BBB in the tumor vasculature, resulting in loss of tumor detectability in Gd-DTPA MRI. However, due to decreased blood volume, treated tumors could be readily detected in USPIO-enhanced MRI scans. Our findings suggest that Gd-DTPA MRI results in overestimation of the effect of antiangiogenic therapy of glioma and that USPIO-MRI provides an important complementary diagnostic tool to evaluate response to antiangiogenic therapy of these tumors.
机译:使用对比增强磁共振成像(CE-MRI)正确描述神经胶质瘤在神经肿瘤学中存在问题。弥散性浸润性生长区域的血脑屏障(BBB)可能完好无损,从而排除了造影剂二乙tri三胺五乙酸(Gd-DTPA)的渗出和随后的MR检测。用抗血管生成化合物治疗可能会使肿瘤检测更加复杂,因为此类化合物可以恢复血管生成区域的血脑屏障。用抗血管生成化合物治疗神经胶质瘤的临床试验越来越多,这要求开发替代的成像方式。在这里,我们调查了使用超小氧化铁颗粒(USPIO,Sinerem)作为血池造影剂的CE-MRI对于检测裸鼠脑胶质瘤是否具有附加价值。我们在携带原位U87胶质瘤的小鼠中比较了传统的T1加权Gd-DTPA增强的MRI与T2 *加权USPIO增强的MRI,这些小鼠经或未经抗血管生成化合物vandetanib(ZD6474,ZACTIMA)治疗。在未经治疗的动物中,肿瘤内的血管渗漏和相对较高的肿瘤血容量分别通过Gd-DTPA和USPIO增强MRI产生了良好的MRI可见性。与先前的发现一致,vandetanib治疗可恢复肿瘤脉管系统中的BBB,从而导致Gd-DTPA MRI中肿瘤的可检测性下降。但是,由于血容量减少,在USPIO增强的MRI扫描中可以轻松检测到已治疗的肿瘤。我们的发现表明,Gd-DTPA MRI导致高估了神经胶质瘤抗血管生成治疗的效果,而USPIO-MRI提供了重要的补充诊断工具来评估对这些肿瘤的抗血管生成治疗的反应。

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