A-803467 is a tetrodotoxin-resistant Nav1.8 sodium channel blocker which can block human Nav1.8 with an IC50 of 8nM [1, 2]. A-803467 can effectively block experimental inflammatory and neuropathic pain caused by the Nav1.8 channel [1].
A-803467 (7.5μM; 2h) enhanced the intracellular [3H]-MX accumulation in ABCG2-transfected HEK293 cells [2]; A-803467 (7.5μM; 0, 30, 60, 120min) significantly blocked the intracellular [3H]-MX efflux from ABCG2-transfected cells [2]; A-803467 (100nM) caused significant current blocking in HEK-293 cells expressing the human Nav1.8 sodium channel [1]; A-803467 (30nM) shortened action potential in mouse ventricular myocytes at slow frequency (0.1Hz) stimulus current [3]; A-803467 (30nM; 15min) reduced frequency of diastolic Ca2+ waves in human atrial cardiomyocytes from patients with sinus rhythm [4].
A-803467 (10, 30, 100mg/kg; i.p.) potently reduced thermal hyperalgesia in the complete Freund’s adjuvant (CFA) Sprague-Dawley (SD) rat model of inflammatory pain [1]; A-803467 (10, 30, 100mg/kg; i.p.) reduced mechanical allodynia in the L5/L6 spinal nerve injury model of SD rats [1]; A-803467 (10, 30, 100mg/kg; i.p.) reduced mechanical allodynia in the chronic constriction injury of the sciatic nerve model of SD rats [1]; A-803467 (10mg/rat; i.a.) reduced joint pain of male Wistar rats which induced by monoiodoacetate (MIA) [5].
References:
[1] Jarvis M F, Honore P, Shieh C C, et al. A-803467, a potent and selective Nav1.8 sodium channel blocker, attenuates neuropathic and inflammatory pain in the rat [J]. Proceedings of the National Academy of Sciences of the United States of America, 2007, 104(20): 8520-8525.
[2] Anreddy N, Patel A, Zhang Y K, et al. A-803467, a tetrodotoxin-resistant sodium channel blocker, modulates ABCG2-mediated MDR in vitro and in vivo [J]. Oncotarget, 2015, 6(36): 39276-39291.
[3] Yang T, Atack T C, Stroud D M, et al. Blocking Scn10a channels in heart reduces late sodium current and is antiarrhythmic [J]. Circulation research, 2012, 111(3): 322-332.
[4] Pabel S, Ahmad S, Tirilomis P, et al. Inhibition of Nav1.8 prevents atrial arrhythmogenesis in human and mice [J]. Basic research in cardiology, 2020, 115(2): 20.
[5] Schuelert N, McDougall J J. Involvement of Nav1.8 sodium ion channels in the transduction of mechanical pain in a rodent model of osteoarthritis [J]. Arthritis research & therapy, 2012, 14(1): R5.
A-803467是一种河豚毒素耐受型Nav1.8钠通道的阻断剂,其阻断人Nav1.8钠通道的IC50为8nM[1, 2]。A-803467可以有效阻断Nav1.8 通道导致的实验性炎症和神经性疼痛[1]。
A-803467(7.5μM;2h)增加了ABCG2转染的HEK293细胞内[3H]-MX的积累[2];A-803467(7.5μM;0、30、60、120min)显著阻断ABCG2转染的HEK293细胞内的[3H]-MX外流[2];A-803467(100nM)使表达人Nav1.8钠通道的HEK-293细胞产生了明显的电流阻滞[1];A-803467 (30nM)在慢频率(0.1Hz)的刺激电流下可以缩短小鼠心室肌细胞的动作电位[3];A-803467 (30nM;15min)降低了窦性心律患者的人心房心肌细胞的舒张压 Ca2+波频率[4]。
A-803467(10、30、100mg/kg;i.p.)可以有效减轻CFA(complete Freund’s adjuvant)诱导的SD大鼠(Sprague-Dawley)炎症性疼痛模型的热痛觉过敏[1];A-803467(10、30、100mg/kg;i.p,)可减轻L5/L6脊髓神经损伤SD大鼠模型的触诱发痛[1];A-803467(10、30、100mg/kg;i.p,)可减轻坐骨神经慢性收缩损伤SD大鼠模型的触诱发痛[1];A-803467(10mg/只;i.a.)可以减轻MIA(monoiodoacetate)诱导的雄性Wistar大鼠的关节疼痛[5]。