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培养的猪主动脉平滑肌细胞中ATP诱导的Ca2+瞬变动力学取决于ATP浓度和储存的Ca2+。

Kinetics of ATP-induced Ca2+ transients in cultured pig aortic smooth muscle cells depend on ATP concentration and stored Ca2+.

作者信息

Kalthof B, Bechem M, Flocke K, Pott L, Schramm M

机构信息

Institute for Cardiovascular and Arteriosclerosis Research, Bayer AG, Wuppertal, FRG.

出版信息

J Physiol. 1993 Jul;466:245-62.

Abstract
  1. Single cultured pig aortic smooth muscle cells were studied using fura-2 and dual excitation wavelength microfluometry. 2. Extracellular ATP in micromolar concentrations induced a transient increase of [Ca2+]i due to Ca2+ release from internal stores. In the same concentration range application of ATP resulted in an increase of intracellular inositol phosphate level. 3. In a medium range of ATP concentrations (2-10 microM) the Ca2+ signal was oscillating, whereas at higher and lower concentrations only a Ca2+ transient with a single peak was elicited. 4. The rank order of potency for the tested purine and pyrimidine nucleotides was: UTP > ATP > ADP >> AMP = adenosine = alpha,beta-methylene ATP = 0. The response to the nucleotides could be abolished by the P2-purinoceptor antagonist suramin. 5. The latency between agonist application and onset of the Ca2+ transients as well as their amplitude and rate of rise are dependent on ATP concentration. 6. Removal of Ca2+ from the extracellular solution led to a progressive decrease of amplitude and prolonged latency of the Ca2+ transients. This shows that depletion of the Ca2+ stores affects kinetics of the ATP-induced Ca2+ release. 7. The inorganic Ca(2+)-influx blockers Ni2+ and Co2+ affected amplitude and latency in a manner similar to Ca2+ removal, while the Ca2+ antagonist nifedipine was ineffective up to a concentration of 10(-6) M. 8. These results reveal a dual dependency of the InsP3-induced Ca2+ release on agonist concentration and filling state of the Ca2+ stores, which supports the hypothesis of a feedback amplification between InsP3 and released Ca2+.
摘要
  1. 使用fura-2和双激发波长显微荧光测定法对单培养的猪主动脉平滑肌细胞进行了研究。2. 微摩尔浓度的细胞外ATP由于从内部储存库释放Ca2+而导致[Ca2+]i短暂增加。在相同浓度范围内应用ATP导致细胞内肌醇磷酸水平升高。3. 在ATP浓度的中等范围内(2 - 10 microM),Ca2+信号呈振荡状态,而在较高和较低浓度时仅引发具有单个峰值的Ca2+瞬变。4. 所测试的嘌呤和嘧啶核苷酸的效力顺序为:UTP > ATP > ADP >> AMP = 腺苷 = α,β-亚甲基ATP = 0。对核苷酸的反应可被P2嘌呤受体拮抗剂苏拉明消除。5. 激动剂应用与Ca2+瞬变开始之间的延迟以及它们的幅度和上升速率取决于ATP浓度。6. 从细胞外溶液中去除Ca2+导致Ca2+瞬变的幅度逐渐降低且延迟延长。这表明Ca2+储存库的耗尽会影响ATP诱导的Ca2+释放的动力学。7. 无机Ca(2+)-内流阻滞剂Ni2+和Co2+对幅度和延迟的影响方式与去除Ca2+类似,而Ca2+拮抗剂硝苯地平在浓度高达10(-6) M时无效。8. 这些结果揭示了InsP3诱导的Ca2+释放对激动剂浓度和Ca2+储存库充盈状态的双重依赖性,这支持了InsP3与释放的Ca2+之间存在反馈放大的假设。

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