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Multiple ryanodine receptor subtypes and heterogeneous ryanodine receptor-gated Ca 2+ stores in pulmonary arterial smooth muscle cells

机译:多种兰尼碱受体亚型和异质性兰尼碱受体门控Ca 2+储存在肺动脉平滑肌细胞中

摘要

Ryanodine receptors (RyRs) of pulmonary arterial smooth muscle cells (PASMCs) play important roles in major physiological processes such as hypoxic pulmonary vasoconstriction and perinatal pulmonary vasodilatation. Recent studies show that three subtypes of RyRs are coexpressed and RyR-gated Ca 2+ stores are distributed heterogeneously in systemic vascular myocytes. However, the molecular identity and subcellular distribution of RyRs have not been examined in PASMCs. In this study we detected mRNA and proteins of all three subtypes in rat intralobar PASMCs using RT-PCR and Western blot. Quantitative real-time RT-PCR showed that RyR2 mRNA was most abundant, ∼15-20 times more than the other two subtypes. Confocal fluorescence microscopy revealed that RyRs labeled with BODIPY TR-X ryanodine were localized in the peripheral and perinuclear regions and were colocalized with sarcoplasmic reticulum labeled with Fluo-5N. Immunostaining showed that the subsarcolemmal regions exhibited clear signals of RyR1 and RyR2, whereas the perinuclear compartments contained mainly RyR1 and RyR3. Ca 2+ sparks were recorded in both regions, and their activities were enhanced by a subthreshold concentration of caffeine or by endothelin-1, indicating functional RyR-gated Ca 2+ stores. Moreover, 18% of the perinuclear sparks were prolonged [full duration/half-maximum (FDHM) = 193.3 ± 22.6 ms] with noninactivating kinetics, in sharp contrast to the typical fast inactivating Ca 2+ sparks (FDHM = 44.6 ± 3.2 ms) recorded in the same PASMCs. In conclusion, multiple RyR subtypes are expressed differentially in peripheral and perinuclear RyR-gated Ca 2+ stores; the molecular-complexity and spatial heterogeneity of RyRs may facilitate specific Ca 2+ regulation of cellular functions in PASMCs. Copyright © 2005 the American Physiological Society.
机译:肺动脉平滑肌细胞(PASMC)的Ryanodine受体(RyRs)在主要生理过程(例如低氧性肺血管收缩和围产期肺血管扩张)中起重要作用。最近的研究表明,RyR的三种亚型是共表达的,并且RyR门控的Ca 2+存储在系统性血管心肌细胞中异质分布。但是,尚未在PASMC中检查RyR的分子同一性和亚细胞分布。在这项研究中,我们使用RT-PCR和Western blot检测了大鼠肺叶PASMCs中所有三种亚型的mRNA和蛋白。实时定量RT-PCR显示RyR2 mRNA最丰富,比其他两个亚型多15〜20倍。共聚焦荧光显微镜检查显示,用BODIPY TR-X ryanodine标记的RyRs定位在外周和核周区域,并与用Fluo-5N标记的肌质网共定位。免疫染色显示,肌膜下区域显示出清晰的RyR1和RyR2信号,而核周区室主要包含RyR1和RyR3。在这两个区域均记录了Ca 2+火花,其咖啡因浓度低于阈值浓度或内皮素-1增强了其活性,表明RyR门控的Ca 2+存储功能良好。此外,18%的核周火花被延长[完整持续时间/半最大值(FDHM)= 193.3±22.6 ms],具有非灭活动力学,与典型的快速灭活Ca 2+火花(FDHM = 44.6±3.2 ms)形成鲜明对比记录在相同的PASMC中。总之,多种RyR亚型在外周和核周RyR门控的Ca 2+贮藏库中差异表达。 RyRs的分子复杂性和空间异质性可能促进PASMCs细胞功能的特定Ca 2+调节。版权所有©2005美国生理学会。

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