腺苷通过A2A受体调节大鼠嗜铬细胞瘤PC12细胞中的缺氧诱导反应。
Adenosine modulates hypoxia-induced responses in rat PC12 cells via the A2A receptor.
作者信息
Kobayashi S, Conforti L, Pun R Y, Millhorn D E
机构信息
Department of Molecular and Cellular Physiology, University of Cincinnati, 231 Bethesda Avenue, PO Box 576, Cincinnati, OH 45267-576, USA.
出版信息
J Physiol. 1998 Apr 1;508 ( Pt 1)(Pt 1):95-107. doi: 10.1111/j.1469-7793.1998.095br.x.
Abstract
- The present study was undertaken to determine the role of adenosine in mediating the cellular responses to hypoxia in rat phaeochromocytoma (PC12) cells, an oxygen-sensitive clonal cell line. 2. Reverse transcriptase polymerase chain reaction studies revealed that PC12 cells express adenosine deaminase (the first catalysing enzyme of adenosine degradation) and the A2A and A2B adenosine receptors, but not the A1 or A3 adenosine receptors. 3. Whole-cell current- and voltage-clamp experiments showed that adenosine attenuated the hypoxia-induced membrane depolarization. The hypoxia-induced suppression of the voltage-sensitive potassium current (IK(V)) was markedly reduced by adenosine. Furthermore, extracellularly applied adenosine increased the peak amplitudes of IK(V) in a concentration-dependent manner. This increase was blocked by pretreatment not only with a non-specific adenosine receptor antagonist, 8-phenyltheophylline (8-PT), but also with a selective A2A receptor antagonist, ZM241385. 4. Ca2+ imaging studies using fura-2 acetoxymethyl ester (fura-2 AM) revealed that the increase in intracellular free Ca2+ during hypoxic exposure was attenuated significantly by adenosine. Voltage-clamp studies showed that adenosine inhibited the voltage-dependent Ca2+ currents (ICa) in a concentration-dependent fashion. This inhibition was also abolished by both 8-PT and ZM241385. 5. The modulation of both IK(V) and ICa by adenosine was prevented by intracellular application of an inhibitor of protein kinase A (PKA), PKA inhibitor fragment (6-22) amide. In addition, the effect of adenosine on either IK(V) or ICa was absent in PKA-deficient PC12 cells. 6. These results indicate that the modulatory effects of adenosine on the hypoxia-induced membrane responses of PC12 cells are likely to be mediated via activation of the A2A receptor, and that the PKA pathway is required for these modulatory actions. We propose that this modulation serves to regulate membrane excitability in PC12 cells and possibly other oxygen-sensitive cells during hypoxia.
摘要
- 本研究旨在确定腺苷在介导大鼠嗜铬细胞瘤(PC12)细胞(一种对氧敏感的克隆细胞系)对缺氧的细胞反应中的作用。2. 逆转录聚合酶链反应研究表明,PC12细胞表达腺苷脱氨酶(腺苷降解的首个催化酶)以及A2A和A2B腺苷受体,但不表达A1或A3腺苷受体。3. 全细胞膜片钳电流和电压钳实验表明,腺苷减弱了缺氧诱导的膜去极化。腺苷显著减轻了缺氧诱导的电压敏感性钾电流(IK(V))的抑制。此外,细胞外施加的腺苷以浓度依赖的方式增加了IK(V)的峰值幅度。这种增加不仅被非特异性腺苷受体拮抗剂8-苯基茶碱(8-PT)预处理所阻断,也被选择性A2A受体拮抗剂ZM241385所阻断。4. 使用fura-2乙酰氧甲酯(fura-2 AM)的Ca2+成像研究表明,缺氧暴露期间细胞内游离Ca2+的增加被腺苷显著减弱。电压钳研究表明,腺苷以浓度依赖的方式抑制电压依赖性Ca2+电流(ICa)。这种抑制也被8-PT和ZM241385所消除。5. 腺苷对IK(V)和ICa的调节作用被细胞内应用蛋白激酶A(PKA)抑制剂PKA抑制片段(6 - 22)酰胺所阻止。此外,在PKA缺陷的PC12细胞中,腺苷对IK(V)或ICa均无作用。6. 这些结果表明,腺苷对PC12细胞缺氧诱导的膜反应的调节作用可能是通过A2A受体的激活介导的,并且PKA途径是这些调节作用所必需的。我们提出这种调节作用有助于在缺氧期间调节PC12细胞以及可能其他对氧敏感的细胞的膜兴奋性。
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