Munro Gordon, Christensen Jeppe K, Erichsen Helle K, Dyhring Tino, Demnitz Joachim, Dam Eva, Ahring Philip K
NeuroSearch A/S, Ballerup, Denmark.
Saniona A/S, Ballerup, Denmark.
CNS Neurosci Ther. 2016 Feb;22(2):135-45. doi: 10.1111/cns.12487. Epub 2015 Dec 10.
Here, we investigate the pharmacology of NS383, a novel small molecule inhibitor of acid-sensing ion channels (ASICs).
ASIC inhibition by NS383 was characterized in patch-clamp electrophysiological studies. Analgesic properties were evaluated in four rat behavioral models of pain.
NS383 inhibited H(+)-activated currents recorded from rat homomeric ASIC1a, ASIC3, and heteromeric ASIC1a+3 with IC50 values ranging from 0.61 to 2.2 μM. However, NS383 was completely inactive at homomeric ASIC2a. Heteromeric receptors containing AISC2a, such as ASIC1a+2a and ASIC2a+3, were only partially inhibited, presumably as a result of stoichiometry-dependent binding. NS383 (10-60 mg/kg, i.p.), amiloride (50-200 mg/kg, i.p.), acetaminophen (100-400 mg/kg, i.p.), and morphine (3-10 mg/kg, i.p.) all dose-dependently attenuated nocifensive behaviors in the rat formalin test, reversed pathological inflammatory hyperalgesia in complete Freund's adjuvant-inflamed rats, and reversed mechanical hypersensitivity in the chronic constriction injury model of neuropathic pain. However, in contrast to acetaminophen and morphine, motor function was unaffected by NS383 at doses at least 8-fold greater than those that were effective in pain models, whilst analgesic doses of amiloride were deemed to be toxic.
NS383 is a potent and uniquely selective inhibitor of rat ASICs containing 1a and/or 3 subunits. It is well tolerated and capable of reversing pathological painlike behaviors, presumably via peripheral actions, but possibly also via actions within central pain circuits.
在此,我们研究了新型酸敏感离子通道(ASICs)小分子抑制剂NS383的药理学特性。
在膜片钳电生理研究中对NS383抑制ASIC的作用进行了表征。在四种大鼠疼痛行为模型中评估了其镇痛特性。
NS383抑制从大鼠同源ASIC1a、ASIC3以及异源ASIC1a + 3记录到的H⁺激活电流,IC50值范围为0.61至2.2 μM。然而,NS383对同源ASIC2a完全无活性。含有AISC2a的异源受体,如ASIC1a + 2a和ASIC2a + 3,仅受到部分抑制,推测是由于化学计量依赖性结合所致。NS383(10 - 60 mg/kg,腹腔注射)、阿米洛利(50 - 200 mg/kg,腹腔注射)、对乙酰氨基酚(100 - 400 mg/kg,腹腔注射)和吗啡(3 - 10 mg/kg,腹腔注射)在大鼠福尔马林试验中均剂量依赖性地减轻伤害性反应行为,逆转完全弗氏佐剂致炎大鼠的病理性炎症性痛觉过敏,并逆转神经病理性疼痛慢性压迫损伤模型中的机械性超敏反应。然而,与对乙酰氨基酚和吗啡不同的是,在剂量至少比对疼痛模型有效的剂量大8倍时,NS383对运动功能无影响,而镇痛剂量的阿米洛利被认为具有毒性。
NS383是一种对含有1a和/或3亚基的大鼠ASICs具有强效且独特选择性的抑制剂。它耐受性良好,能够逆转病理性疼痛样行为,推测是通过外周作用,但也可能通过中枢疼痛回路内的作用实现。