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The response of human retinal pigmented epithelial cells in vitro to changes in nitric oxide concentration stimulated by low levels of red light

机译:低水平红光刺激的人视网膜色素上皮细胞在体外响应氧化物浓度的变化

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The goal of this project is to explore the role of nitric oxide (NO) in regulating the response of hTERT-RPE to low-level exposures to red light. Exposure to low-level red light has been shown to positively affect wound healing, reduce pain, and encourage cell proliferation. The current explanation for this effect is described as an interaction between the photons and cytochrome c oxidase (Cco), which plays a role in regulation of intracellular NO levels in addition to being the mitochondrial protein complex where reduction of oxygen occurs in the process of oxidative phosphorylation. Exposure to 2.88 J/cm2 of 671-nm and 637-nm light shows a two-fold increase in NO immediately after exposure, and a 56% increase in ATP measured at ~5 h post exposure. Levels of NF-κB mRNA and protein were measured at six and 24 h, respectively, and found to increase six fold, correlating with increases in NO levels. Light-stimulated increased levels of NO also correlated with an 11-fold increase in Bcl-2 and a 70% decrease in Bax mRNA levels, relative to controls. NF-κB promotes cell growth and Bcl-2 is an apoptosis suppressor protein. Bax is a positive apoptotic effector protein. These results support the hypothesis that light-induced changes in the intracellular levels of NO play a role in the beneficial effects of low-level light photobiomodulation
机译:该项目的目的是探讨一氧化氮(NO)调节HTERT-RPE对低水平曝光的响应的作用。暴露于低水平的红光已经显示出积极影响伤口愈合,减少疼痛,并促进细胞增殖。这种效果的目前的说明被描述为光子和细胞色素C氧化酶(CCO)之间的相互作用,除了作为线粒体蛋白质复合物的细胞内蛋白质复合物在氧化过程中发生的线粒体蛋白质复合物之外,在细胞内没有水平的调节中起作用。磷酸化。暴露于2.88 j / cm 2的671纳米和637纳米光显示出暴露后立即出现两倍,并且在暴露后约5小时测量ATP的56%增加。在6和24小时的情况下测量NF-κBmRNA和蛋白质的水平,发现增加了六倍,与无水平的增加相关。相对于对照,光刺激的增加的含量不与Bcl-2的11倍的增加和70%降低的70%。 NF-κB促进细胞生长,Bcl-2是凋亡抑制蛋白。 Bax是阳性凋亡效应蛋白。这些结果支持的假设,即在低水平光光生物调节的有益效果中发挥着内细胞内水平的光引起的变化

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