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Non-blocking modulation contributes to sodium channel inhibition by a covalently attached photoreactive riluzole analog

机译:非阻塞调节通过共价附着的光反应反应性Riluzole类似物有助于钠通道抑制作用

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Sodium channel inhibitor drugs decrease pathological hyperactivity in various diseases including pain syndromes, myotonia, arrhythmias, nerve injuries and epilepsies. Inhibiting pathological but not physiological activity, however, is a major challenge in drug development. Sodium channel inhibitors exert their effects by a dual action: they obstruct ion flow (“block”), and they alter the energetics of channel opening and closing (“modulation”). Ideal drugs would be modulators without blocking effect, because modulation is inherently activity-dependent, therefore selective for pathological hyperactivity. Can block and modulation be separated? It has been difficult to tell, because the effect of modulation is obscured by conformation-dependent association/dissociation of the drug. To eliminate dynamic association/dissociation, we used a photoreactive riluzole analog which could be covalently bound to the channel; and found, unexpectedly, that drug-bound channels could still conduct ions, although with modulated gating. The finding that non-blocking modulation is possible, may open a novel avenue for drug development because non-blocking modulators could be more specific in treating hyperactivity-linked diseases.
机译:钠通道抑制剂药物在各种疾病中降低病理过度活性,包括疼痛综合征,肌肌肌肌肌肌肌炎,心律失常,神经损伤和癫痫。然而,抑制病理但不是生理活动,是药物发展中的主要挑战。钠通道抑制剂通过双重作用施加它们的效果:它们阻碍了离子流量(“块”),并且它们改变了通道开启和关闭的能量学(“调制”)。理想的药物是调节剂而不会阻塞效果,因为调节本质上是活性依赖性的,因此有选择病理过度活性。可以阻止和调制分开?它难以告诉,因为调节的效果是通过依赖于药物的构象依赖性/解离来模糊的。为了消除动态关联/解离,我们使用了光度反应性的riilzole类似物,其可以与通道共价结合;并且出乎意料地发现,这种药物结合的通道仍然可以进行离子,尽管用调制门控。未阻断调制是可能的,可以打开一种新颖的药物开发途径,因为非阻塞调节剂可以更具体地治疗多动链接疾病。

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