Psychological and Brain Sciences (X.L., A.S.D., M.H., K.M., A.G.H.), Program in Neuroscience (K.M., A.G.H.), and Gill Center for Biomolecular Science (K.M., A.G.H.), Indiana University, Bloomington, Indiana.
Psychological and Brain Sciences (X.L., A.S.D., M.H., K.M., A.G.H.), Program in Neuroscience (K.M., A.G.H.), and Gill Center for Biomolecular Science (K.M., A.G.H.), Indiana University, Bloomington, Indiana
Mol Pharmacol. 2018 Feb;93(2):49-62. doi: 10.1124/mol.117.109355. Epub 2017 Nov 30.
The CB cannabinoid agonist LY2828360 lacked both toxicity and efficacy in a clinical trial for osteoarthritis. Whether LY2828360 suppresses neuropathic pain has not been reported, and its signaling profile is unknown. In vitro, LY2828360 was a slowly acting but efficacious G protein-biased CB agonist, inhibiting cAMP accumulation and activating extracellular signal-regulated kinase 1/2 signaling while failing to recruit arrestin, activate inositol phosphate signaling, or internalize CB2 receptors. In wild-type (WT) mice, LY2828360 (3 mg/kg per day i.p. × 12 days) suppressed chemotherapy-induced neuropathic pain produced by paclitaxel without producing tolerance. Antiallodynic efficacy of LY2828360 was absent in CB knockout (KO) mice. Morphine (10 mg/kg per day i.p. × 12 days) tolerance developed in CBKO mice but not in WT mice with a history of LY2828360 treatment (3 mg/kg per day i.p. × 12 days). LY2828360-induced antiallodynic efficacy was preserved in WT mice previously rendered tolerant to morphine (10 mg/kg per day i.p. × 12 days), but it was absent in morphine-tolerant CBKO mice. Coadministration of LY2828360 (0.1 mg/kg per day i.p. × 12 days) with morphine (10 mg/kg per day × 12 days) blocked morphine tolerance in WT but not in CBKO mice. WT mice that received LY2828360 coadministered with morphine exhibited a trend ( = 0.055) toward fewer naloxone-precipitated jumps compared with CBKO mice. In conclusion, LY2828360 is a slowly signaling, G protein-biased CB agonist that attenuates chemotherapy-induced neuropathic pain without producing tolerance and may prolong effective opioid analgesia while reducing opioid dependence. LY2828360 may be useful as a first-line treatment in chemotherapy-induced neuropathic pain and may be highly efficacious in neuropathic pain states that are refractive to opioid analgesics.
LY2828360 是一种 CB 大麻素激动剂,在治疗骨关节炎的临床试验中既没有毒性也没有疗效。LY2828360 是否抑制神经病理性疼痛尚未报道,其信号转导谱也不清楚。体外研究表明,LY2828360 是一种作用缓慢但有效的 G 蛋白偏向性 CB 激动剂,抑制 cAMP 积累并激活细胞外信号调节激酶 1/2 信号通路,而不招募阻滞蛋白,激活肌醇磷酸信号通路,或内化 CB2 受体。在野生型(WT)小鼠中,LY2828360(每天腹腔注射 3mg/kg,共 12 天)抑制紫杉醇引起的化疗诱导的神经病理性疼痛,而不产生耐受。LY2828360 在 CB 敲除(KO)小鼠中没有抗痛觉过敏作用。吗啡(每天腹腔注射 10mg/kg,共 12 天)在 CBKO 小鼠中产生耐受,但在 LY2828360 治疗(每天腹腔注射 3mg/kg,共 12 天)史的 WT 小鼠中没有产生耐受。在先前对吗啡(每天腹腔注射 10mg/kg,共 12 天)耐受的 WT 小鼠中,LY2828360 诱导的抗痛觉过敏作用得到保留,但在吗啡耐受的 CBKO 小鼠中则没有。LY2828360(每天腹腔注射 0.1mg/kg,共 12 天)与吗啡(每天腹腔注射 10mg/kg,共 12 天)联合给药阻断了 WT 小鼠但未阻断 CBKO 小鼠的吗啡耐受。接受 LY2828360 联合吗啡治疗的 WT 小鼠与 CBKO 小鼠相比,纳洛酮诱发的跳跃次数有减少的趋势(=0.055)。总之,LY2828360 是一种缓慢信号转导的 G 蛋白偏向性 CB 激动剂,可减轻化疗诱导的神经病理性疼痛而不产生耐受,并可能延长有效的阿片类镇痛作用,同时减少阿片类药物依赖。LY2828360 可作为化疗诱导的神经病理性疼痛的一线治疗药物,对于对阿片类镇痛药有反应的神经病理性疼痛状态可能具有高度疗效。
