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首页> 外文期刊>Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology >Specific binding of 2-(125I)iodomelatonin by rat splenocytes: characterization and its role on regulation of cyclic AMP production.
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Specific binding of 2-(125I)iodomelatonin by rat splenocytes: characterization and its role on regulation of cyclic AMP production.

机译:大鼠脾细胞对2-(125I)卵磷脂的特异性结合:表征及其在调节环AMP产生中的作用。

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In the present paper we show that pineal hormone melatonin interacts with rat splenocytes through high-affinity binding sites. Binding of 2-[125I]iodomelatonin ([125I]MEL) by splenocytes fulfills all criteria for binding to a receptor site. Binding exhibited properties such as dependence on time and temperature as well as reversibility, saturability, high affinity, specificity, and increased under constant light exposure. Results suggest binding to a single class of binding sites without cooperative interactions. The dissociation constant (Kd) for the single site was 0.34 nM with a binding capacity of 2.25 fmol/10(7) cells. These data are in close agreement with data obtained from kinetic studies, in which the kinetically derived value of the dissociation constant was 0.20 nM. The affinity of these binding sites suggests that they may recognize the physiological concentrations of melatonin in serum. Moreover, pharmacological doses of melatonin also inhibited cyclic AMP production stimulated by forskolin, a potent activator of adenylate cyclase system. The demonstration of [125I]MEL binding sites in the spleen, in addition to those described in blood mononuclear cells and thymus, provides evidence to support a direct mechanism of action of melatonin on immune system.
机译:在本文中,我们显示松果激素褪黑激素通过高亲和力结合位点与大鼠脾细胞相互作用。脾细胞与2- [125I]碘弹性蛋白([125I] MEL)的结合符合与受体位点结合的所有标准。结合表现出诸如对时间和温度的依赖性以及可逆性,饱和性,高亲和力,特异性和在恒定曝光下增加的性质。结果表明结合到单一种类的结合位点而没有协同相互作用。单个位点的解离常数(Kd)为0.34 nM,结合能力为2.25 fmol / 10(7)细胞。这些数据与从动力学研究获得的数据非常吻合,在动力学研究中,解离常数的动力学衍生值为0.20 nM。这些结合位点的亲和力表明它们可以识别血清中褪黑激素的生理浓度。此外,褪黑激素的药理剂量也抑制了福司可林(腺苷酸环化酶系统的有效活化剂)刺激的环状AMP产生。除了在血液单核细胞和胸腺中描述的那些之外,在脾脏中的[125I] MEL结合位点的证明提供了支持褪黑激素对免疫系统直接作用机制的证据。

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