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用一组磷光氧敏探针评估细胞内氧梯度。

Assessment of cellular oxygen gradients with a panel of phosphorescent oxygen-sensitive probes.

机构信息

Biochemistry Department, University College Cork, Cork, Ireland.

出版信息

Anal Chem. 2012 Mar 20;84(6):2930-8. doi: 10.1021/ac3000144. Epub 2012 Feb 29.

Abstract

The supply of oxygen (O(2)) to respiring tissue, cells, and mitochondria regulates metabolism, gene expression, and cell fate. Depending on the cell type and mitochondrial function, O(2) gradients between extra- and intracellular compartments may vary and play important physiological roles such as the regulation of activity of prolyl hydroxylases and adaptive responses to hypoxia. Here we present a new methodology for the analysis of localized O(2) gradients in cultures of adherent cells, using three phosphorescent Pt-porphyrin based probes with different localization. One new O(2) probe targeted to the cell membrane was developed and used together with existing MitoXpress and Nano2 probes to monitor mean pericellular (PC), extracellular (EC), and intracellular (IC) O(2) concentrations, respectively. Mouse fibroblasts and neuronal PC12 cells cultured in standard microplates were stained with probes and measured on a commercial time-resolved fluorescence reader in phosphorescence lifetime mode. Respiring cells exposed to various levels of atmospheric O(2) showed differences in oxygenation of their IC, PC, and EC compartments. Experiments with different cell numbers and modulation of respiration activity demonstrated that these gradients are dynamic and regulated by the O(2) diffusion and consumption rate. The new method facilitates the assessment of such gradients.

摘要

氧气(O(2))供应(respiring tissue, cells, 和 mitochondria)调节代谢、基因表达和细胞命运。根据细胞类型和线粒体功能的不同,细胞内外间隙的 O(2)梯度可能会有所不同,并发挥重要的生理作用,如脯氨酰羟化酶活性的调节和对低氧的适应性反应。在这里,我们提出了一种新的方法,用于分析粘附细胞培养物中局部 O(2)梯度,使用三种基于不同定位的磷光 Pt-卟啉探针。开发了一种新的靶向细胞膜的 O(2)探针,与现有的 MitoXpress 和 Nano2 探针一起,分别用于监测细胞周腔(PC)、细胞外(EC)和细胞内(IC)的平均 O(2)浓度。用探针染色培养在标准微孔板中的小鼠成纤维细胞和神经元 PC12 细胞,并在商业时间分辨荧光读取器上以磷光寿命模式进行测量。暴露于不同大气 O(2)水平的呼吸细胞显示其 IC、PC 和 EC 隔室的氧合作用存在差异。不同细胞数量的实验和呼吸活性的调节表明这些梯度是动态的,并受 O(2)扩散和消耗速率的调节。新方法有助于评估这些梯度。

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