Changes in perfusion and permeability in glioblastoma model induced by the anti-angiogenic agents cediranib and thalidomide.

IF 2.7 3区 医学 Q3 ONCOLOGY Acta Oncologica Pub Date : 2024-08-14 DOI:10.2340/1651-226X.2024.40116
Jérôme Conq, Nicolas Joudiou, Véronique Préat, Bernard Gallez
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Abstract

Background and purpose: The poor delivery of drugs to infiltrating tumor cells contributes to therapeutic failure in glioblastoma. During the early phase of an anti-angiogenic treatment, a remodeling of the tumor vasculature could occur, leading to a more functional vessel network that could enhance drug delivery. However, the restructuration of blood vessels could increase the proportion of normal endothelial cells that could be a barrier for the free diffusion of drugs. The net balance, in favor or not, of a better delivery of compounds during the course of an antiangiogenic treatment remains to be established. This study explored whether cediranib and thalidomide could modulate perfusion and vessel permeability in the brain U87 tumor mouse model.

Methods: The dynamic evolution of the diffusion of agents outside the tumor core using the fluorescent dye Evans Blue in histology and Gd-DOTA using dynamic contrast-enhanced (DCE)-MRI. CD31 labelling of endothelial cells was used to measure the vascular density.

Results and interpretation: Cediranib and thalidomide effectively reduced tumor size over time. The accessibility of Evans Blue outside the tumor core continuously decreased over time. The vascular density was significantly decreased after treatment while the proportion of normal vessels remained unchanged over time. In contrast to histological studies, DCE-MRI did not tackle any significant change in hemodynamic parameters, in the core or margins of the tumor, whatever the parameter used or the pharmacokinetic model used. While cediranib and thalidomide were effective in decreasing the tumor size, they were ineffective in transiently increasing the delivery of agents in the core and the margins of the tumor.

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抗血管生成药物西地尼布和沙利度胺诱导胶质母细胞瘤模型灌注和渗透性的变化
背景和目的:对浸润肿瘤细胞的药物输送不畅是胶质母细胞瘤治疗失败的原因之一。在抗血管生成治疗的早期阶段,肿瘤血管可能会发生重塑,从而形成功能性更强的血管网络,从而促进药物的输送。然而,血管的重构可能会增加正常内皮细胞的比例,从而阻碍药物的自由扩散。在抗血管生成治疗过程中,是否能更好地输送化合物,仍有待确定。本研究探讨了西地尼布和沙利度胺是否能调节脑 U87 肿瘤小鼠模型的灌注和血管通透性:方法:在组织学中使用荧光染料埃文斯蓝,在动态对比增强(DCE)-MRI中使用Gd-DOTA,对肿瘤核心外的药物扩散进行动态演化。内皮细胞的CD31标记用于测量血管密度:结果与解释:随着时间的推移,西地尼布和沙利度胺能有效缩小肿瘤。随着时间的推移,埃文斯蓝在肿瘤核心外的可及性不断降低。治疗后血管密度明显降低,而正常血管的比例随时间推移保持不变。与组织学研究不同的是,无论使用何种参数或药代动力学模型,DCE-MRI 均未发现肿瘤核心或边缘的血液动力学参数有任何显著变化。虽然西地尼布和沙利度胺能有效缩小肿瘤大小,但它们却不能有效地瞬时增加肿瘤核心和边缘的药物输送。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Acta Oncologica
Acta Oncologica 医学-肿瘤学
CiteScore
4.30
自引率
3.20%
发文量
301
审稿时长
3 months
期刊介绍: Acta Oncologica is a journal for the clinical oncologist and accepts articles within all fields of clinical cancer research. Articles on tumour pathology, experimental oncology, radiobiology, cancer epidemiology and medical radio physics are also welcome, especially if they have a clinical aim or interest. Scientific articles on cancer nursing and psychological or social aspects of cancer are also welcomed. Extensive material may be published as Supplements, for which special conditions apply.
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