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A DNA vaccine targeting angiomotin inhibits angiogenesis and suppresses tumor growth

机译:靶向血管动蛋白的DNA疫苗抑制血管生成并抑制肿瘤生长

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摘要

Endogenous angiogenesis inhibitors have shown promise in preclinical trials, but clinical use has been hindered by low half-life in circulation and high production costs. Here, we describe a strategy that targets the angiostatin receptor angiomotin (Amot) by DNA vaccination. The vaccination procedure generated antibodies that detected Amot on the endothelial cell surface. Purified Ig bound to the endothelial cell membrane and inhibited endothelial cell migration. In vivo, DNA vaccination blocked angiogenesis in the matrigel plug assay and prevented growth of transplanted tumors for up to 150 days. We further demonstrate that a combination of DNA vaccines encoding Amot and the extracellular and transmembrane domains of the human EGF receptor 2 (Her-2)/neu oncogene inhibited breast cancer progression and impaired tumor vascularization in Her-2/neu transgenic mice. No toxicity or impairment of normal blood vessels could be detected. This work shows that DNA vaccination targeting Amot may be used to mimic the effect of angiostatin.
机译:内源性血管生成抑制剂已在临床前试验中显示出希望,但由于循环半衰期低和生产成本高,阻碍了临床应用。在这里,我们描述了一种通过DNA疫苗靶向血管抑制素受体血管动蛋白(Amot)的策略。疫苗接种程序产生了在内皮细胞表面检测到Amot的抗体。纯化的Ig结合到内皮细胞膜并抑制内皮细胞迁移。在体内,DNA疫苗在基质胶栓试验中阻止了血管生成,并在长达150天的时间内阻止了移植肿瘤的生长。我们进一步证明,编码Amot的DNA疫苗以及人EGF受体2(Her-2)/ neu癌基因的胞外和跨膜结构域的组合可抑制乳腺癌的进展并损害Her-2 / neu转基因小鼠的肿瘤血管形成。没有检测到正常血管的毒性或损伤。这项工作表明靶向Amot的DNA疫苗接种可用于模拟血管抑制素的作用。

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