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Steroid inhibition of erythrocyte-derived ATP reduces endothelial cell production of nitric oxide in a 3D-printed fluidic model

机译:在3D打印的流体模型中,类固醇抑制红细胞衍生的ATP减少了一氧化氮的内皮细胞生成

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Multiple sclerosis (MS) is a disease of the central nervous system affecting over 2.5 million people worldwide. MS is characterized by blood brain barrier (BBB) damage and demyelination of axons, which causes brain lesions leading to complications such as numbness and blurred vision. Steroid medications are available to help treat symptoms of MS, and although the mechanism of action of steroids is known for most cells, it is not completely understood with respect to red blood cells (RBCs). Here, we show that the steroids estriol and prednisolone effect RBC ATP release and downstream endothelial NO production, which may be a mechanism of action of steroids in the bloodstream. Our results suggest that while RBCs obtained from people with MS release significantly more ATP than RBCs from healthy people (healthy: 216 ± 11 nM, MS: 321 ± 18 nM), a significant decrease up to 183 nM in ATP release is measured due to the presence of physiological levels of estriol or prednisolone. Further analysis measured a 31% decrease in endothelial nitric oxide (NO) production from endothelial cells in contact with RBCs treated with estriol or prednisolone. These results suggest that steroids may have an additional mechanism of action in the bloodstream through their ability to attenuate RBC ATP release. ATP stimulates NO production in vivo, and while high levels of NO are detrimental to the BBB, it follows that hindering the amount of ATP in the bloodstream would decrease the BBB damage and demyelination in MS.
机译:多发性硬化症(MS)是一种中枢神经系统疾病,影响了全世界250万人。 MS的特征在于血脑屏障(BBB)损伤和轴突脱髓鞘,其引起脑损伤,导致诸如麻木和视力模糊的并发症。类固醇药物可以帮助治疗MS症状,尽管大多数细胞都知道类固醇的作用机理,但对于红细胞(RBC)尚不完全了解。在这里,我们表明类固醇雌三醇和泼尼松龙影响RBC ATP释放和下游内皮一氧化氮的产生,这可能是类固醇在血流中的作用机制。我们的结果表明,尽管从MS患者获得的RBC释放的ATP比健康人的RBC显着多(健康:216±11 nM,MS:321±18 nM),但是由于以下原因,ATP释放显着降低至183 nM:雌三醇或泼尼松龙的生理水平的存在。进一步的分析表明,与雌三醇或泼尼松龙处理的RBC接触后,内皮细胞产生的内皮一氧化氮(NO)减少了31%。这些结果表明,类固醇通过减弱RBC ATP释放的能力,可能在血流中具有其他作用机制。 ATP刺激体内NO的产生,而高水平的NO对BBB有害,因此可以得出结论,阻碍血液中ATP的含量将减少MS中BBB的损伤和脱髓鞘。

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