Adenosine receptors in basolateral membranes of rat renal cortex.

Z Jakubowski, R Skowroński, A Matecki, D Mohuczy, T Pawełczyk, J Stepiński, S Angielski
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Abstract

High affinity binding sites for adenosine were identified in rat kidney cortex basolateral membranes. Kinetic analysis indicates two sets of [3H]adenosine, [3H]ADO, binding sites, one with high affinity and Kd = 0.84 +/- 0.25 microM, one with low affinity and Kd = 4.74 +/- 0.37 microM. The ADO receptors were further characterized using ADO analogs as binding inhibitors. The most potent inhibitor of [3H]ADO binding was N-methyl-adenosine with a Kd of 5 microM, whereas 2-deoxyadenosine was about 50 times less potent. The binding of [3H]phenylisopropyladenosine, [3H]PIA, and [3H]-N-ethylcarboxamidoadenosine, [3H]NECA, to basolateral membranes was rapid and reversible. The Scatchard plot of [3H]PIA binding showed monophasic curves for experiments performed at 0 degrees C and 37 degrees C. The apparent Kd of [3H]PIA binding at 0 degrees C was 0.19 +/- 0.05 nM and 0.34 +/- 0.07 nM at 37 degrees C. The binding of [3H]NECA to basolateral membranes was found with an apparent affinity Kd of 110 +/- 50 nM at 0 degrees C. Pretreatment of membranes with N-ethylmaleimide (NEM) inhibited the [3H]PIA binding and did not affect the [3H]NECA binding. These results demonstrate that both A1 and A2 adenosine receptors are present in basolatertal membranes of rat kidney.

大鼠肾皮质基底外膜腺苷受体。
在大鼠肾皮质基底外膜中发现了腺苷的高亲和力结合位点。动力学分析表明有两组[3H]腺苷,[3H]ADO,结合位点,一组高亲和力,Kd = 0.84 +/- 0.25微米,一组低亲和力,Kd = 4.74 +/- 0.37微米。用ADO类似物作为结合抑制剂进一步表征ADO受体。[3H]ADO结合最有效的抑制剂是n -甲基腺苷,Kd为5微米,而2-脱氧腺苷的抑制作用约为50倍。[3H]苯基异丙基腺苷[3H]PIA和[3H]- n -乙基羧氨基腺苷[3H]NECA与基底外侧膜的结合是快速和可逆的。的Scatchard阴谋[3 h] PIA绑定显示单相曲线实验在0摄氏度,37度C [3 h]明显Kd PIA绑定在0摄氏度为0.19 + / - 0.05和0.34 + / - 0.07 nM 37度C [3 h] NECA的绑定基底外侧膜被发现明显的亲和力Kd 110 + / - 50 nM 0度C预处理的膜N-ethylmaleimide (NEM)抑制[3 h] PIA绑定,不影响[3 h] NECA绑定。这些结果表明,A1和A2腺苷受体均存在于大鼠肾基底侧膜中。
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