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血管内皮生长因子165的过表达驱动肿瘤周围间质对流并诱导淋巴引流:磁共振成像、共聚焦显微镜检查以及三标记白蛋白的组织学追踪

Overexpression of vascular endothelial growth factor 165 drives peritumor interstitial convection and induces lymphatic drain: magnetic resonance imaging, confocal microscopy, and histological tracking of triple-labeled albumin.

作者信息

Dafni Hagit, Israely Tomer, Bhujwalla Zaver M, Benjamin Laura E, Neeman Michal

机构信息

Department of Biological Regulation, Weizmann Institute of Science, Rehovot, 76100 Israel.

出版信息

Cancer Res. 2002 Nov 15;62(22):6731-9.

Abstract

Increased expression of vascular endothelial growth factor (VEGF) has been associated with increased lymph node metastases. The aim of this work was to determine whether VEGF-induced hyperpermeability affects peritumor interstitial convection and lymphatic drain, thus linking this growth factor with lymphatic function. Noninvasive imaging of lymphatic function induced by vascular hyperpermeability was achieved by following the distribution of albumin triple-labeled with biotin, fluorescein, and gadolinium-diethylene triamine pentaacetic acid. This contrast material allowed for multimodality imaging using magnetic resonance imaging (MRI), confocal microscopy, and histology. Overexpression of VEGF in C6-pTET-VEGF165 tumors, inoculated in hind limbs of nude mice, elevated vascular permeability, interstitial convection, and lymphatic drain. These were manifested in dynamic MRI measurements by outward flux of the contrast material, the rate of which correlated with tumor volume followed by directional flow toward the popliteal lymph node. Avidin-chase, namely i.v. administration of avidin, was applied for inducing rapid clearance of the intravascular biotinylated contrast material, thus allowing early experimental separation between vascular leak and lymphatic drain. Repeated MRI measurements of the same mice were conducted 48 h after withdrawal of VEGF by addition of tetracycline to the drinking water. VEGF withdrawal decreased tumor blood-plasma volume fraction by 43%, reduced tumor permeability by 75%, and abolished interstitial convection of the contrast material. Histological sections and whole-mount confocal microscopy confirmed VEGF-induced changes in permeability and interstitial accumulation of the contrast material, as well as uptake of the contrast material into peritumor lymphatic vessels. These results revealed a direct link between expression of VEGF165 and peritumor lymphatic drain, thus suggesting a possible role for tumor-derived VEGF in metastatic spread to sentinel lymph nodes.

摘要

血管内皮生长因子(VEGF)表达增加与淋巴结转移增多有关。本研究的目的是确定VEGF诱导的高通透性是否会影响肿瘤周围间质对流和淋巴引流,从而将这种生长因子与淋巴功能联系起来。通过追踪生物素、荧光素和钆-二乙烯三胺五乙酸三重标记的白蛋白分布,实现了对血管高通透性诱导的淋巴功能的无创成像。这种造影剂允许使用磁共振成像(MRI)、共聚焦显微镜和组织学进行多模态成像。接种于裸鼠后肢的C6-pTET-VEGF165肿瘤中VEGF的过表达提高了血管通透性、间质对流和淋巴引流。这些在动态MRI测量中表现为造影剂的外向通量,其速率与肿瘤体积相关,随后造影剂向腘窝淋巴结定向流动。抗生物素蛋白追踪,即静脉注射抗生物素蛋白,用于诱导血管内生物素化造影剂的快速清除,从而在早期实验中区分血管渗漏和淋巴引流。在饮用水中添加四环素撤除VEGF 48小时后,对同一只小鼠进行重复的MRI测量。撤除VEGF使肿瘤血-浆体积分数降低43%,肿瘤通透性降低75%,并消除了造影剂的间质对流。组织学切片和整装共聚焦显微镜证实了VEGF诱导的造影剂通透性变化和间质积聚,以及造影剂被肿瘤周围淋巴管摄取。这些结果揭示了VEGF165表达与肿瘤周围淋巴引流之间的直接联系,从而提示肿瘤来源的VEGF在转移至前哨淋巴结中的可能作用。

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