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首页> 外文期刊>Purinergic signalling >2a€2,3a€2-Emphasis Type="Italic"O/Emphasis-Substituted ATP derivatives as potent antagonists of purinergic P2X3 receptors and potential analgesic agents
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2a€2,3a€2-Emphasis Type="Italic"O/Emphasis-Substituted ATP derivatives as potent antagonists of purinergic P2X3 receptors and potential analgesic agents

机译:2a€2,3a€2- O -取代的ATP衍生物作为嘌呤能P2X3受体和潜在止痛剂的有效拮抗剂

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摘要

Blocking membrane currents evoked by the activation of purinergic P2X3 receptors localized on nociceptive neurons represents a promising strategy for the development of agents useful for the treatment of chronic pain conditions. Among compounds endowed with such antagonistic action, 2a€2,3a€2-O-(2,4,6-trinitrophenyl)-ATP (TNP-ATP) is an ATP analogue, whose inhibitory activity on P2X receptors has been previously reported. Based on the results of molecular modelling studies performed with homology models of the P2X3 receptor, novel adenosine nucleotide analogues bearing cycloalkyl or arylalkyl substituents replacing the trinitrophenyl moiety of TNP-ATP were designed and synthesized. These new compounds were functionally evaluated on native P2X3 receptors from mouse trigeminal ganglion (TG) sensory neurons using patch clamp recordings under voltage clamp configuration. Our data show that some of these molecules are potent (nanomolar range) and reversible inhibitors of P2X3 receptors, without any apparent effect on trigeminal GABAA and 5-HT3 receptors, whose membrane currents were unaffected by the tested compounds.
机译:通过定位在伤害性神经元上的嘌呤能P2X3受体的激活而引起的阻断膜电流代表了开发可用于治疗慢性疼痛状况的药物的有希望的策略。在具有这种拮抗作用的化合物中,2a€2,3a€2- O -(2,4,6-三硝基苯基)-ATP(TNP-ATP) ,其对P2X受体的抑制活性已有报道。基于对P2X3受体的同源性模型进行的分子建模研究的结果,设计并合成了带有环烷基或芳烷基取代基取代TNP-ATP的三硝基苯基部分的新型腺苷核苷酸类似物。使用电压钳配置下的膜片钳记录,对来自小鼠三叉神经节(TG)感觉神经元的天然P2X3受体进行了功能评估。我们的数据表明,其中一些分子是有效的(纳摩尔级)和可逆的P2X3受体抑制剂,对三叉神经GABA A 和5-HT 3 受体没有明显作用,其膜电流不受测试化合物的影响。

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