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Nitric Oxide-donating Derivatives of Chrysin Stimulate Angiogenesis and Upregulating VEGF Production

机译:Chrysin的一氧化氮衍生物刺激血管生成和上调VEGF生产

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Angiogenesis, the development of new capillaries from pre-existing vessels, requires the coordinate activation of endothelial cells, which migrate and proliferate to form functional vessels. Endothelial dysfunction and decreased nitric oxide bioavailability may underscore the impairment of angiogenesis. As such, the delivery of exogenous NO is an attractive therapeutic option that has been used to therapeutic angiogenesis. In this paper, a novel group of hybrid nitric oxide-releasing chrysin derivatives was synthesized. The results indicated that all these chrysin derivatives exhibited promotion of endothelial migration and tubulogenesis in vitro as well as stimulation angiogenesis in vivo. Furthermore, all compounds released NO upon incubation with phosphate buffer at pH 7.4 and enhanced VEGF secretion and VEGF mRNA expression of endothelial cells. These hybrid ester NO donor prodrugs offer a potential drug design concept for the development of therapeutic or preventive agents for angiogenesis deficiency due to ischemic diseases.
机译:血管生成,来自预先存在的血管的新毛细血管的发展需要坐标活化内皮细胞,其迁移和增殖形成功能血管。内皮功能障碍和一氧化氮生物利用度降低可能强调血管生成的损伤。因此,外源性的递送是一种有吸引力的治疗选择,用于治疗血管生成。本文合成了一种新型的杂化杂交氧化物释放蛹衍生物。结果表明,所有这些Chrysin衍生物在体外促进内皮迁移和小管发生以及体内刺激血管生成。此外,所有化合物在pH7.4的pH 7.4下培养时释放不释放,并增强VEGF分泌和内皮细胞的VEGF mRNA表达。这些杂种酯没有供体前药物提供潜在的药物设计理念,用于缺血性疾病导致血管生成缺乏的治疗或预防剂的发展。

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