Sensitive angiogenesis imaging of orthotopic bladder tumors in mice using a selective magnetic resonance imaging contrast agent containing VEGF121/rGel.

Cho EJ; Yang J; Mohamedali KA; Lim EK; Kim EJ; Farhangfar CJ; Suh JS; Haam S; Rosenblum MG; Huh YM

首页> 外文期刊>Investigative radiology >Sensitive angiogenesis imaging of orthotopic bladder tumors in mice using a selective magnetic resonance imaging contrast agent containing VEGF121/rGel.

【24h】

Sensitive angiogenesis imaging of orthotopic bladder tumors in mice using a selective magnetic resonance imaging contrast agent containing VEGF121/rGel.

机译：使用包含VEGF121 / rGel的选择性磁共振成像造影剂对小鼠原位膀胱肿瘤进行敏感的血管生成成像。

获取原文

获取原文并翻译 | 示例

获取外文期刊封面目录资料

开具论文收录证明 >>

文献代查 >>

文献数据库（团队版） >>

页面导航

摘要
著录项
引文网络
相似文献
相关主题

摘要

OBJECTIVES: To investigate the efficiency of magnetic resonance imaging (MRI) contrast agents employing vascular endothelial growth factor (VEGF121)/rGel conjugated MnFe2O4 nanocrystals for imaging of neovasculature using a bladder tumor model. MATERIALS AND METHODS: VEGF121/rGel was conjugated to MnFe2O4 nanoparticles (MNPs). The targeting efficiency and detection capability of the VEGF121/rGel-MNPs were investigated in both KDR-deficient (253JB-V) and KDR-overexpressing (PAE/KDR) cells using MRI. The internalization of VEGF121/rGel-MNPs into cells was confirmed by electron microscopy. Their phosphorylation ability and cytotoxicity were compared with unconjugated VEGF121/rGel. The orthotopic tumor mice were established by implanting low KDR-expressing 253JB-V cells into the bladder dome. After tail-vein injection of VEGF121/rGel-MNPs, the MR signal enhancement of intratumoral vessels by VEGF121/rGel-MNPs was observed and inhibition test using VEGF121 was also conducted. Ex vivo MR imaging of tumor tissue, and a fluorescence immunostaining study was also performed. RESULTS: The water-soluble VEGF121/rGel-MNPs (44.5 +/- 1.2 nm) were stably suspended in the biologic media and exhibited a high relaxivity coefficient (423 mMs). They demonstrated sufficient targeting capability against KDR-overexpressing PAE/KDR cells, as confirmed by dose-dependent MR images and VEGF121 inhibition tests. The phosphorylation activity of KDR and cytotoxicity of VEGF121/rGel-MNPs were evaluated. VEGF121/rGel-MNPs successfully targeted the tumor and provided accurate anatomic details through (i) acquisition of clear neoangiogenic vascular distributions and (ii) obvious enhancement of the MR signal in T2*-weighted images. Immunostaining and blocking studies demonstrated the specific targeting ability of VEGF121/rGel-MNPs toward intratumoral angiogenesis. CONCLUSIONS: Synthesized VEGF121/rGel-MNPs as targeted MR imaging contrast agents can be specifically delivered to tumors and bind to KDR-expressing angiogenic tumor vessels.

机译：目的：研究使用血管内皮生长因子（VEGF121）/ rGel共轭的MnFe2O4纳米晶体的磁共振成像（MRI）造影剂在膀胱肿瘤模型中对新血管成像的效率。材料与方法：VEGF121 / rGel与MnFe2O4纳米颗粒（MNPs）共轭。使用MRI研究了KDR缺陷（253JB-V）和KDR过表达（PAE / KDR）细胞中VEGF121 / rGel-MNP的靶向效率和检测能力。通过电子显微镜确认了VEGF121 / rGel-MNPs向细胞的内在化。将其磷酸化能力和细胞毒性与未结合的VEGF121 / rGel进行了比较。通过将表达低KDR的253JB-V细胞植入膀胱穹顶，建立原位肿瘤小鼠。尾静脉注射VEGF121 / rGel-MNPs后，观察到VEGF121 / rGel-MNPs增强了肿瘤内血管的MR信号，并进行了VEGF121抑制试验。还进行了肿瘤组织的离体MR成像和荧光免疫染色研究。结果：水溶性VEGF121 / rGel-MNPs（44.5 +/- 1.2 nm）稳定地悬浮在生物介质中，并具有较高的弛豫系数（423 mMs）。他们证明了针对过表达KDR的PAE / KDR细胞的足够的靶向能力，这一点已通过剂量依赖性MR图像和VEGF121抑制测试得到证实。评价了KDR的磷酸化活性和VEGF121 / rGel-MNP的细胞毒性。 VEGF121 / rGel-MNPs成功地靶向肿瘤并通过（i）获取清晰的新血管生成血管分布和（ii）在T2 *加权图像中MR信号明显增强提供了准确的解剖学细节。免疫染色和阻断研究证明了VEGF121 / rGel-MNPs对肿瘤内血管生成的特异性靶向能力。结论：合成的VEGF121 / rGel-MNPs作为靶向MR成像造影剂可特异性递送至肿瘤，并与表达KDR的血管生成肿瘤血管结合。

著录项

来源
《Investigative radiology》 |2011年第7期|共9页
作者
Cho EJ; Yang J; Mohamedali KA; Lim EK; Kim EJ; Farhangfar CJ; Suh JS; Haam S; Rosenblum MG; Huh YM;
展开▼
作者单位

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类放射医学;
关键词

相似文献

外文文献
中文文献
专利

1. Sensitive angiogenesis imaging of orthotopic bladder tumors in mice using a selective magnetic resonance imaging contrast agent containing VEGF121/rGel. [J] . Cho EJ, Yang J, Mohamedali KA, Investigative radiology . 2011,第7期

机译：使用包含VEGF121 / rGel的选择性磁共振成像造影剂对小鼠原位膀胱肿瘤进行敏感的血管生成成像。
2. Molecular imaging of tumor-associated angiogenesis using a novel magnetic resonance imaging contrast agent targeting αvβ3 integrin [J] . DeberghI., VanDammeN., DeNaeyerD., Annals of surgical oncology . 2014,第6期

机译：使用靶向αvβ3整联蛋白的新型磁共振成像造影剂对肿瘤相关血管生成进行分子成像
3. Tumor Characterization with Dynamic Contrast Enhanced Magnetic Resonance Imaging and Biodegradable Macromolecular Contrast Agents in Mice [J] . Xueming Wu, Yi Feng, Eun-Kee Jeong, Pharmaceutical Research . 2009,第9期

机译：动态对比增强磁共振成像和可生物降解的大分子对比剂在小鼠中的肿瘤表征。
4. Sterically Stabilized Magnetoliposomes as Contrast Agents for in vivo Magnetic Resonance Imaging andTherapy of Solid Tumors [C] . Marie-Sophie Martina, Jean-Paul Fortin, Christine Ménager, Annual meeting exposition of the Controlled Release Society . 2005

机译：立体稳定的磁脂质体作为体内磁共振成像和实体瘤治疗的对比剂
5. The assessment of brain tumor angiogenesis using susceptibility contrast agent-based functional magnetic resonance imaging. [D] . Pathak, Arvind Pratap. 2001

机译：使用基于敏感性对比剂的功能磁共振成像评估脑肿瘤血管生成。
6. Characterization of Tumor Angiogenesis with Dynamic Contrast Enhanced Magnetic Resonance Imaging and Biodegradable Macromolecular Contrast Agents in Mice [O] . Yi Feng, Eun-Kee Jeong, Aaron M. Mohs, -1

机译：动态对比增强磁共振成像和可生物降解的大分子对比剂对小鼠肿瘤血管生成的表征。
7. Molecular imaging of tumor-associated angiogenesis using a novel magnetic resonance imaging contrast agent targeting αvβ3 integrin [O] . DEBERGH ISABELLE, Van Damme Nancy, De Naeyer Dieter, 2014

机译：使用靶向αvβ3整联蛋白的新型磁共振成像造影剂的肿瘤相关血管生成的分子成像

Sensitive angiogenesis imaging of orthotopic bladder tumors in mice using a selective magnetic resonance imaging contrast agent containing VEGF121/rGel.

摘要

著录项

引文网络

相似文献

相关主题

期刊订阅