首页> 美国卫生研究院文献>Frontiers in Aging Neuroscience >The generation of induced pluripotent stem cells for macular degeneration as a drug screening platform: identification of curcumin as a protective agent for retinal pigment epithelial cells against oxidative stress
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The generation of induced pluripotent stem cells for macular degeneration as a drug screening platform: identification of curcumin as a protective agent for retinal pigment epithelial cells against oxidative stress

机译:黄斑变性诱导多能干细胞的产生作为药物筛选平台:姜黄素作为视网膜色素上皮细胞抗氧化应激的保护剂的鉴定

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摘要

Age-related macular degeneration (AMD) is one retinal aging process that may lead to irreversible vision loss in the elderly. Its pathogenesis remains unclear, but oxidative stress inducing retinal pigment epithelial (RPE) cells damage is perhaps responsible for the aging sequence of retina and may play an important role in macular degeneration. In this study, we have reprogrammed T cells from patients with dry type AMD into induced pluripotent stem cells (iPSCs) via integration-free episomal vectors and differentiated them into RPE cells that were used as an expandable platform for investigating pathogenesis of the AMD and in-vitro drug screening. These patient-derived RPEs with the AMD-associated background (AMD-RPEs) exhibited reduced antioxidant ability, compared with normal RPE cells. Among several screened candidate drugs, curcumin caused most significant reduction of ROS in AMD-RPEs. Pre-treatment of curcumin protected these AMD-RPEs from H2O2-induced cell death and also increased the cytoprotective effect against the oxidative stress of H2O2 through the reduction of ROS levels. In addition, curcumin with its versatile activities modulated the expression of many oxidative stress-regulating genes such as PDGF, VEGF, IGFBP-2, HO1, SOD2, and GPX1. Our findings indicated that the RPE cells derived from AMD patients have decreased antioxidative defense, making RPE cells more susceptible to oxidative damage and thereby leading to AMD formation. Curcumin represented an ideal drug that can effectively restore the neuronal functions in AMD patient-derived RPE cells, rendering this drug an effective option for macular degeneration therapy and an agent against aging-associated oxidative stress.
机译:年龄相关性黄斑变性(AMD)是一种视网膜衰老过程,可能导致老年人不可逆转的视力丧失。其发病机理尚不清楚,但氧化应激诱导视网膜色素上皮细胞(RPE)的损伤可能是视网膜老化的原因,并且可能在黄斑变性中起重要作用。在这项研究中,我们已通过无整合游离型载体将干型AMD患者的T细胞重编程为诱导性多能干细胞(iPSC),并将它们分化为RPE细胞,将其用作研究AMD和肝癌发病机制的可扩展平台。 -体外药物筛选。与正常RPE细胞相比,这些具有AMD相关背景的患者衍生RPE(AMD-RPE)表现出降低的抗氧化能力。在几种筛选的候选药物中,姜黄素引起AMD-RPEs中ROS的最大减少。姜黄素的预处理可保护这些AMD-RPE免受H2O2诱导的细胞死亡,并通过降低ROS水平提高了针对H2O2氧化应激的细胞保护作用。此外,姜黄素具有多种活性,可调节许多氧化应激调节基因的表达,例如PDGF,VEGF,IGFBP-2,HO1,SOD2和GPX1。我们的发现表明,源自AMD患者的RPE细胞的抗氧化防御能力降低,从而使RPE细胞更容易受到氧化损伤,从而导致AMD的形成。姜黄素代表了一种理想的药物,可以有效地恢复AMD患者来源的RPE细胞的神经元功能,使该药物成为黄斑变性治疗的有效选择,并且是抗衰老相关氧化应激的药物。

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