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斑马鱼血管生成:一种药物筛选的新模型。

Zebrafish angiogenesis: a new model for drug screening.

作者信息

Serbedzija G N, Flynn E, Willett C E

机构信息

Phylonix Pharmaceuticals, Inc., Cambridge, MA 02139, USA.

出版信息

Angiogenesis. 1999;3(4):353-9. doi: 10.1023/a:1026598300052.

DOI:10.1023/a:1026598300052
PMID:14517415
Abstract

Angiogenesis is necessary for tumor growth, making inhibition of vessel formation an excellent target for cancer therapy. Current assays for angiogenesis, however, are too complex to be practical for drug screening. Here, we demonstrate that the zebrafish is a viable whole animal model for screening small molecules that affect blood vessel formation. Blood vessel patterning is highly characteristic in the developing zebrafish embryo and the subintestinal vessels (SIVs) can be stained and visualized microscopically as a primary screen for compounds that affect angiogenesis. Small molecules added directly to the fish culture media diffuse into the embryo and induce observable, dose-dependent effects. To evaluate the zebrafish as a model, we used two angiogenesis inhibitors, SU5416 and TNP470, both of which have been tested in mammalian systems. Both compounds caused a reduction in vessel formation when introduced to zebrafish embryos prior to the onset of angiogenesis. Short duration (1 h) exposure of SU5416 was sufficient to block new angiogenic and vasculogenic vessel formation. In contrast, TNP470 required continuous exposure to block SIV formation and had no apparent effect on vasculogenic vessel formation. To ascertain whether blood vessels in the zebrafish embryo respond to angiogenic compounds, we introduced human VEGF into embryos. Injection of VEGF caused an observable increase in SIV formation.

摘要

血管生成是肿瘤生长所必需的,这使得抑制血管形成成为癌症治疗的一个理想靶点。然而,目前用于血管生成的检测方法过于复杂,不适用于药物筛选。在此,我们证明斑马鱼是一种可行的整体动物模型,可用于筛选影响血管形成的小分子。在发育中的斑马鱼胚胎中,血管模式具有高度特征性,肠下血管(SIVs)可以被染色并通过显微镜观察,作为筛选影响血管生成化合物的初步筛选方法。直接添加到鱼类培养基中的小分子会扩散到胚胎中,并诱导出可观察到的、剂量依赖性的效应。为了评估斑马鱼作为一种模型,我们使用了两种血管生成抑制剂SU5416和TNP470,这两种抑制剂都已在哺乳动物系统中进行过测试。当在血管生成开始之前将这两种化合物引入斑马鱼胚胎时,都会导致血管形成减少。短时间(1小时)暴露于SU5416足以阻断新的血管生成和血管发生性血管形成。相比之下,TNP470需要持续暴露才能阻断SIV形成,并且对血管发生性血管形成没有明显影响。为了确定斑马鱼胚胎中的血管是否对血管生成化合物有反应,我们将人血管内皮生长因子(VEGF)引入胚胎中。注射VEGF导致SIV形成明显增加。

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