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首页> 外文期刊>Heart failure reviews >A sustained-release drug-delivery system of synthetic prostacyclin agonist, ONO-1301SR: a new reagent to enhance cardiac tissue salvage and/or regeneration in the damaged heart
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A sustained-release drug-delivery system of synthetic prostacyclin agonist, ONO-1301SR: a new reagent to enhance cardiac tissue salvage and/or regeneration in the damaged heart

机译:合成前列环素激动剂ONO-1301SR的缓释药物递送系统:一种增强受损组织中心脏组织挽救和/或再生的新试剂

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Cardiac failure is a major cause of mortality and morbidity worldwide, since the standard treatment for cardiac failure in the clinical practice is chiefly to focus on removal of insults against the heart or minimisation of additional factors to exacerbate cardiac failure, but not on regeneration of the damaged cardiac tissue. A synthetic prostacyclin agonist, ONO-1301, has been developed as a long-acting drug for acute and chronic pathologies related to regional ischaemia, inflammation and/or interstitial fibrosis by pre-clinical studies. In addition, poly-lactic co-glycolic acid-polymerised form of ONO-1301, ONO-1301SR, was generated to achieve a further sustained release of this drug into the targeted region. This unique reagent has been shown to act on fibroblasts, vascular smooth muscle cells and endothelial cells in the tissue via the prostaglandin IP receptor to exert paracrinal release of multiple protective factors, such as hepatocyte growth factor, vascular endothelial growth factor or stromal cell-derived factor-1, into the adjacent damaged tissue, which is salvaged and/or regenerated as a result. Our laboratory developed a new surgical approach to treat acute and chronic cardiac failure using a variety of animal models, in which ONO-1301SR is directly placed over the cardiac surface to maximise the therapeutic effects and minimise the systemic complications. This review summarises basic and pre-clinical information of ONO-1301 and ONO-1301SR as a new reagent to enhance tissue salvage and/or regeneration, with a particular focus on the therapeutic effects on acute and chronic cardiac failure and underlying mechanisms, to explore a potential in launching the clinical study.
机译:心力衰竭是全球范围内死亡率和发病率的主要原因,因为在临床实践中,心力衰竭的标准治疗方法主要是着眼于消除对心脏的损害或使加重心力衰竭的其他因素减至最少,而不是心力衰竭的再生。受损的心脏组织。通过临床前研究,已开发出一种合成的前列环素激动剂ONO-1301作为长效药物,用于与局部缺血,炎症和/或间质纤维化有关的急性和慢性病理。此外,生成了ONO-1301的聚乳酸共乙醇酸聚合形式ONO-1301SR,以实现该药物向目标区域的进一步持续释放。这种独特的试剂已被证明可通过前列腺素IP受体作用于组织中的成纤维细胞,血管平滑肌细胞和内皮细胞,从而在多种细胞内分泌保护因子,如肝细胞生长因子,血管内皮生长因子或基质细胞衍生因子-1进入邻近的受损组织,因此被挽救和/或再生。我们的实验室开发了一种使用多种动物模型治疗急性和慢性心力衰竭的新手术方法,其中将ONO-1301SR直接放置在心脏表面上方以最大程度地发挥治疗作用并最大程度地减少全身并发症。这篇综述总结了ONO-1301和ONO-1301SR作为增强组织挽救和/或再生的新试剂的基本和临床前信息,特别着重于对急性和慢性心力衰竭的治疗作用及其潜在机制,以进行探索。具有开展临床研究的潜力。

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