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首页> 外文期刊>American Journal of Physiology >N-methyl-D-aspartate receptors in human erythroid precursor cells and in circulating red blood cells contribute to the intracellular calcium regulation
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N-methyl-D-aspartate receptors in human erythroid precursor cells and in circulating red blood cells contribute to the intracellular calcium regulation

机译:人类红系前体细胞和循环红细胞中的N-甲基-D-天冬氨酸受体有助于细胞内钙的调节

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摘要

The presence of N-methyl-D-aspartate receptor (NMDAR) was previously shown in rat red blood cells (RBCs) and in a UT-7/Epo human myeloid cell line differentiating into erythroid lineage. Here we have characterized the subunit composition of the NMDAR and monitored its function during human erythropoiesis and in circulating RBCs. Expression of the NMDARs subunits was assessed in erythroid progenitors during ex vivo erythropoiesis and in circulating human RBCs using quantitative PCR and flow cytometry. Receptor activity was monitored using a radiolabeled antagonist binding assay, live imaging of Ca2++ uptake, patch clamp, and monitoring of cell volume changes. The receptor tetramers in erythroid precursor cells are composed of the NR1, NR2A, 2C, 2D, NR3A, and 3B subunits of which the glycine-binding NR3A and 3B and glutamate-binding NR2C and 2D subunits prevailed. Functional receptor is required for survival of erythroid precursors. Circulating RBCs retain a low number of the receptor copies that is higher in young cells compared with mature and senescent RBC populations. In circulating RBCs the receptor activity is controlled by plasma glutamate and glycine. Modulation of the NMDAR activity in RBCs by agonists or antagonists is associated with the alterations in whole cell ion currents. Activation of the receptor results in the transient Ca2++ accumulation, cell shrinkage, and alteration in the intracellular pH, which is associated with the change in hemoglobin oxygen affinity. Thus functional NMDARs are present in erythroid precursor cells and in circulating RBCs. These receptors contribute to intracellular Ca2++ homeostasis and modulate oxygen delivery to peripheral tissues.
机译:N-甲基-D-天冬氨酸受体(NMDAR)的存在先前已在大鼠红细胞(RBC)和分化为红系谱系的UT-7 / Epo人类骨髓细胞系中显示。在这里,我们已经表征了NMDAR的亚基组成,并在人类红细胞生成和循环红细胞中监测了其功能。使用定量PCR和流式细胞术评估离体红细胞生成过程中红系祖细胞和循环人类红细胞中NMDARs亚基的表达。使用放射性标记的拮抗剂结合测定,Ca2 ++摄取的实时成像,膜片钳和细胞体积变化的监测来监测受体活性。红细胞前体细胞中的受体四聚体由NR1,NR2A,2C,2D,NR3A和3B亚基组成,其中结合甘氨酸的NR3A和3B和谷氨酸结合的NR2C和2D亚基占优势。功能受体是红系前体生存所必需的。与成熟和衰老的RBC群体相比,循环的RBC保留了少量的受体拷贝,在年轻细胞中更高。在循环的红细胞中,受体活性受血浆谷氨酸和甘氨酸控制。激动剂或拮抗剂对红细胞中NMDAR活性的调节与全细胞离子流的改变有关。受体的激活导致Ca2 ++的短暂积累,细胞收缩和细胞内pH值的改变,这与血红蛋白氧亲和力的变化有关。因此,功能性NMDAR存在于类红细胞前体细胞和循环RBC中。这些受体有助于细胞内Ca2 ++稳态,并调节氧向周围组织的输送。

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