Department of Physiology, University of Toronto, Canada.
Neuropharmacology. 2010 Jun;58(7):1045-53. doi: 10.1016/j.neuropharm.2010.01.011. Epub 2010 Jan 28.
Acid-sensing ion channels (ASICs) are proton-gated cation channels that are predominantly expressed in the nervous system. ASICs are involved in a number of neurological diseases such as pain, ischemic stroke and multiple sclerosis but limited tools are available to target these channels and provide probes for their physiological functions. Here we report that the anti-protozoal diarylamidines, 4',6-diamidino-2-phenylindole (DAPI), diminazene, hydroxystilbamidine (HSB) and pentamidine potently inhibit ASIC currents in primary cultured hippocampal neurons with apparent affinities of 2.8 microM, 0.3 microM, 1.5 microM and 38 microM, respectively. These four compounds (100 microM) failed to block ENaC channels expressed in oocytes. Sub-maximal concentrations of diminazene also strongly accelerated desensitization of ASIC currents in hippocampal neurons. Diminazene blocked ASIC1a, -1b -2a, and -3 currents expressed in CHO cells with a rank order of potency 1b > 3 > 2a >or= 1a. Patchdock computational analysis suggested a binding site of diarylamidines on ASICs. This study indicates diarylamidines constitute a novel class of non-amiloride ASIC blockers and suggests that diarylamidines may be developed as therapeutic agents in treatment of ASIC-involved diseases.
酸敏离子通道(ASICs)是质子门控阳离子通道,主要表达于神经系统。ASICs 参与多种神经系统疾病,如疼痛、缺血性中风和多发性硬化症,但目前可用的靶向这些通道的工具有限,也缺乏用于研究其生理功能的探针。本文报道抗原生动物的二脒类化合物,4',6-二脒基-2-苯基吲哚(DAPI)、苯脒、羟芐脒(HSB)和戊烷脒,能强烈抑制原代培养海马神经元中的 ASIC 电流,其表观亲和力分别为 2.8μM、0.3μM、1.5μM 和 38μM。这四种化合物(100μM)不能阻断卵母细胞中表达的 ENaC 通道。苯脒的亚最大浓度也能强烈加速海马神经元中 ASIC 电流的脱敏。苯脒在 CHO 细胞中对 ASIC1a、-1b -2a 和 -3 电流的抑制作用具有效力顺序为 1b > 3 > 2a >or= 1a。Patchdock 计算分析表明二脒类化合物在 ASICs 上具有结合位点。本研究表明二脒类化合物构成了一类新型的非阿米洛利 ASIC 阻断剂,并提示二脒类化合物可能被开发为治疗 ASIC 相关疾病的治疗剂。
