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Curcumin- and Cyclopamine-Loaded Liposomes to Enhance Therapeutic Efficacy Against Hepatic Fibrosis

机译:姜黄素和环丙胺加载的脂质体,以提高肝纤维化的治疗效果

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Background and Purpose:Hepatic fibrosis is a public health problem characterized by activation of hepatic stellate cells (HSCs), which triggers excessive production of extracellular matrix (ECM). Inhibition of HSC activation may be an effective treatment. Since various pathways control HSC activation, a combination of drugs with different mechanisms may be more effective than monotherapy.Methods:Here, we prepared liposomes loaded with curcumin and cyclopamine to inhibit HSC activation. We systematically analyzed the physicochemical characteristics of liposomes loaded with the two drugs, as well as their effects on HSC proliferation, activation and collagen production on gene, protein and cellular levels.Results:The prepared liposomes helped solubilize both drugs, contributing to their uptake by cells. Liposomes loaded with both drugs inhibited cell proliferation, migration and invasion, as well as induced more apoptosis and perturbed the cell cycle more than the free combination of both drugs in solution or liposomes loaded with either drug alone. Liposomes loaded with both drugs strongly suppressed HSC activation and collagen secretion.Conclusion:Our results suggest that liposome encapsulation can increase the uptake of curcumin and cyclopamine as well as the synergism between them in anti-fibrosis. This approach shows potential for treating hepatic fibrosis.? 2020 Zhang et al.
机译:背景论:肝纤维化是一种公共健康问题,其特征在于激活肝星状细胞(HSC),其触发过量的细胞外基质(ECM)。 HSC活化的抑制可以是有效的治疗方法。由于各种途径控制HSC活化,具有不同机制的药物组合可能比单疗法更有效。在此,我们在这里制备脂质体加入姜黄素和环丙氨酸以抑制HSC活化。我们系统地分析了用两种药物负荷的脂质体的物理化学特征,以及它们对基因,蛋白质和细胞水平的HSC增殖,活化和胶原蛋白产生的影响。结果:制备的脂质体有助于溶解两种药物,促进其吸收细胞。脂质体含有两种药物的脂质体抑制细胞增殖,迁移和侵袭,以及诱导更多细胞凋亡并扰乱细胞周期,而不是单独加载任何一种药物的溶液或脂质体的自由组合。用两种药物负载的脂质体强制抑制HSC活化和胶原蛋白分泌。结论:我们的结果表明,脂质体包封可以增加姜黄素和环丙胺的摄取以及它们之间的抗纤维化之间的协同作用。这种方法表明了治疗肝纤维化的可能性。 2020张等人。

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