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Intracellular pH (pHin) and cytosolic calcium (Ca2+cyt) regulation via ATPases: studies in cell populations single cells and subcellular compartments

机译:通过ATP酶的细胞内pH(phin)和细胞溶质钙(Ca2 + cyt)调节:在细胞群中的研究单细胞和亚细胞室

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Changes in pH$+in$/ and (Ca$+2$PLU$/)$+cyt$/ are important in the signal transduction mechanisms leading to many physiological responses including cell growth, motility, secretion/exocytosis, etc. The concentrations of these ions are regulated via primary and secondary ion transporting mechanisms. In diabetes, specific pH and Ca$+2$PLU$/ regulatory mechanism might be altered. To study these ions, we employ fluorescence spectroscopy, and cell imagin spectroscopy/confocal microscopy. pH and Ca$+2$PLU$/ indicators are loaded in the cytosol with acetoxymethyl ester forms of dyes, and in endosomal/lysosomal (E/L) compartments by overnight incubation of cells with dextran- conjugated ion fluorescent probes. We focus on specific pH and Ca$+2$PLU$/ regulatory systems: plasmalemmal vacuolar- type H$+$PLU$/-ATPases (pm V-ATPases) and sarcoplasmic/endoplasmic reticulum Ca$+2$PLU$/-ATPases (SERCA). As experimental models, we employ vascular smooth muscle (VSM) and microvascular endothelial cells. We have chosen these cells because they are important in blood flow regulation and in angiogenesis. These processes are altered in diabetes. In many cell types, ion transport processes are dependent on metabolism of glucose for maximal activity. Our main findings are: (a) glycolysis coupling the activity of SERCA is required for cytosolic Ca$+2$PLU$/ homeostasis in both VSM and microvascular endothelial cells; (b) E/L compartments are important for pH and Ca$+2$PLU$/ regulation via H$+$PLU$/-ATPases and SERCA, respectively; and (c) pm-V-ATPases are important for pH$+in$/ regulation in microvascular endothelial cells.
机译:$ /和(CA $ + 2 $ / /)$ + cyt $ /在信号转导机制中的变化导致许多生理反应,包括细胞生长,运动,分泌物/外尿尿量等。浓度这些离子通过初级和二次离子输送机制来调节。在糖尿病中,特定的pH和CA $ + 2 $ /监管机制可能会被改变。为了研究这些离子,我们使用荧光光谱和细胞敏感性/共聚焦显微镜。 PH和CA $ + 2 $ PLU $ /指标用乙酰氧基甲基酯形式的染料和通过用葡聚糖 - 缀合的离子荧光探针孵育细胞过夜的细胞溶剂和内体/溶酶体(E / L)隔室。我们专注于特定的PH和CA $ + 2 $ PLU $ /监管系统:PLASMALEMMAL VACUOLAR-类型H $ + $ PLU $ / - ATPASES(PM V-ATPASES)和肌肉/内质网CA $ + 2 $ PLU $ / - ATPASES(SERCA)。作为实验模型,我们采用血管平滑肌(VSM)和微血管内皮细胞。我们选择了这些细胞,因为它们在血流调节和血管生成中都很重要。这些过程在糖尿病中改变。在许多细胞类型中,离子传输过程取决于葡萄糖的代谢以获得最大活动。我们的主要研究结果是:(a)糖酵解偶联Serca的活性是在VSM和微血管内皮细胞中的细胞溶质CA $ + 2 $ /稳态所必需的; (b)通过H $ + $ PLU $ / - ATPASE和SERCA,E / L隔间对于PH和CA $ + 2 $ /法规非常重要; (c)PM-V-ATP酶对微血管内皮细胞的$ /调节的pH值+至关重要。

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