Tumor necrosis factor (TNF) causes regression of advanced cancers when used in isolation perfusion with melphalan; evidence suggests these effects are mediated via selective yet uncharacterized actions on tumor neovasculature. A novel derivative, colloidal gold bound TNF (cAu-TNF) has been shown to have similar antitumor effects as native TNF with less systemic toxicity in mice. These studies were done to determine their effects on tumor neovasculature, using in vivo video microscopy. Female C57BL/6 mice bearing 20 mm(2) MC38 or LLC tumors that are TNF sensitive and resistant tumors, respectively, had dorsal skinfold chambers implanted. The rate of interstitial accumulation of Texas red fluorescently labeled albumin in tumor and normal vasculature was measured after intravenous TNF, cAu-TNF or PBS. Changes in interstitial fluorescent intensity over time were quantified as a reflection of alterations in vascular permeability. MC38 bearing mice treated with TNF or cAu-TNF demonstrated a rapid, selective and significant increase in tracer accumulation in areas of neovasculature compared to those of normal vasculature. Experiments in LLC tumor bearing mice showed similar results. Monoclonal antibody against tissue factor partially abrogated the effects of TNF on MC38 neovasculature. These data provide direct evidence that TNF and cAu-TNF selectively and rapidly alter permeability in tumor neovasculature; a phenomenon that may be exploited to enhance selective delivery of chemotherapeutics to tumor.

译文

:肿瘤坏死因子(TNF)与美法仑单独灌注使用时可导致晚期癌症消退;证据表明这些作用是通过对肿瘤新脉管系统的选择性但未表征的作用介导的。一种新型衍生物,胶体金结合TNF(cAu-TNF)已显示出与天然TNF相似的抗肿瘤作用,并且对小鼠的全身毒性较小。使用体内视频显微镜,进行了这些研究以确定它们对肿瘤新脉管系统的影响。携带20毫米(2)MC38或LLC肿瘤的雌性C57BL / 6小鼠分别是TNF敏感和耐药性肿瘤,已植入了背部皮褶室。静脉注射TNF,cAu-TNF或PBS后,测量德克萨斯州红色荧光标记白蛋白在肿瘤和正常脉管系统中的间质累积率。间质荧光强度随时间的变化被量化为反映血管通透性变化的反映。与正常脉管系统的小鼠相比,用TNF或cAu-TNF治疗的MC38荷瘤小鼠在示踪剂在新脉管系统区域的蓄积迅速,选择性且显着增加。在LLC荷瘤小鼠中进行的实验显示了相似的结果。针对组织因子的单克隆抗体部分消除了TNF对MC38新脉管系统的影响。这些数据提供了直接的证据,表明TNF和cAu-TNF选择性和迅速地改变了肿瘤新脉管系统的通透性。一种可以用来增强化学疗法向肿瘤的选择性递送的现象。

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