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首页> 外文期刊>American Journal of Physiology >Evidence of synergistic/additive effects of sildenafil and erythropoietin in enhancing survival and migration of hypoxic endothelial cells
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Evidence of synergistic/additive effects of sildenafil and erythropoietin in enhancing survival and migration of hypoxic endothelial cells

机译:西地那非和促红细胞生成素对缺氧内皮细胞存活和迁移的协同/累加作用的证据

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摘要

Endothelial cell dysfunction is a common event to several pathologies including pulmonary hypertension, which is often associated with hypoxia. As the endothelium plays an essential role in regulating the dynamic interaction between pulmonary vasodilata-tion and vasoconstriction, this cell type is fundamental in the development of vascular remodeling and increased vascular resistance. We investigated the protective effects of sildenafil, a phos-phodiesterase type 5 inhibitor, given in combination with erythropoietin (Epo), as it has been demonstrated that both drugs have antiapoptotic effects on several cell types. Specifically, we examined the viability and angiogenic properties of rat pulmonary artery endothelial cells upon exposure to either 21% or 1% oxygen, in presence of sildenafil (1 and 100 nM) and Epo (5 and 20 U/ml) alone or in combination (1 nM and 20 U/mi). Cell proliferation and viability were analyzed by Trypan blue staining, MTT assay, and Annexin V/propidium iodide stainings. In all assays, the ability of the combination treatment in improving cell viability was superior to that of either drug alone. The angiogenic properties were studied using a migration and a 3D collagen assay, and the results revealed increases in the migration potential of endothelial cells as well as the ability to form tube-like structures in response to sildenafil and the combination treatment. We therefore conclude that both drugs exert protective effects on endothelial cells on hypoxia and that sildenafil enhances the migratory and angiogenic properties, especially in hypoxic conditions. Furthermore, we present evidence of possible additive or synergistic effects of both drugs.
机译:内皮细胞功能障碍是包括肺动脉高压在内的多种病理的常见事件,而肺动脉高压通常与缺氧有关。由于内皮在调节肺血管舒张和血管收缩之间的动态相互作用中起着至关重要的作用,因此这种细胞类型在血管重塑和增加的血管阻力中起着至关重要的作用。我们已经研究了5磷酸磷酸二酯酶抑制剂西地那非与促红细胞生成素(Epo)联合给予的保护作用,因为已证明两种药物对几种细胞类型均具有抗凋亡作用。具体来说,我们研究了在单独或联合使用昔多芬(1和100 nM)和Epo(5和20 U / ml)的情况下,暴露于21%或1%的氧气下的大鼠肺动脉内皮细胞的活力和血管生成特性(1 nM和20 U / mi)。通过锥虫蓝染色,MTT测定和膜联蛋白V /碘化丙啶染色分析细胞增殖和活力。在所有测定中,联合治疗改善细胞生存力的能力均优于任何一种药物。使用迁移和3D胶原测定法研究了血管生成特性,结果显示内皮细胞的迁移潜力增加,并且响应西地那非和联合治疗可形成管状结构。因此,我们得出的结论是,这两种药物均对缺氧的内皮细胞产生保护作用,而西地那非可增强迁移和血管生成特性,尤其是在低氧条件下。此外,我们提供了两种药物可能产生加和或协同作用的证据。

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