Centre for Integrated Preclinical Drug Development, School of Biomedical Sciences, Faculty of Medicine, The University of Queensland, Brisbane, QLD, Australia.
Boehringer Ingelheim Pharma GmbH and Co. KG, Biberach, Germany.
Pharmacol Rep. 2020 Oct;72(5):1418-1425. doi: 10.1007/s43440-020-00145-8. Epub 2020 Jul 26.
The pathobiology of prostate cancer-induced bone pain (PCIBP) is underpinned by both inflammatory and neuropathic components. Here, we used a rat model of PCIBP to assess the analgesic efficacy of a glycine transporter 2 (GlyT2) inhibitor (N-(6-((1,3-dihydroxypropan-2-yl)amino)-2-(dimethylamino)pyridin-3-yl)-3,5-dimethoxy-4-(4-(trifluoromethyl)phenoxy) benzamide) relative to two clinically available adjuvant drugs that are recommended for the relief of neuropathic pain, viz, pregabalin and duloxetine.
PCIBP was induced in male Wistar Han rats following intra-tibial injection (ITI) of rat prostate cancer (AT3B) cells into the left tibia. Sham-rats received an ITI of heat-killed AT3B cells. PCIBP rats with fully developed mechanical allodynia in the ipsilateral hindpaws as assessed using von Frey filaments, received single oral (p.o.) bolus doses of the GlyT2 inhibitor (3-30 mg/kg), pregabalin (3-100 mg/kg), duloxetine (3-100 mg/kg), or vehicle. Baseline paw withdrawal thresholds (PWTs) were determined in the ipsilateral (injured side) and contralateral hindpaws immediately prior to dosing and at scheduled times for 3 h post dosing in individual animals.
Single oral bolus doses of the GlyT2 inhibitor (3-30 mg/kg) evoked partial pain relief at the doses tested in the ipsilateral hindpaws of PCIBP rats without any discernible behavioural side effects. By contrast, single oral bolus doses of pregabalin at 10-100 mg/kg evoked dose-dependent and complete alleviation of mechanical allodynia. By comparison, single oral bolus doses of duloxetine at doses up to 100 mg/kg lacked efficacy.
Oral administration of this GlyT2 inhibitor evoked partial pain relief in PCIBP rats and did not evoke central nervous system side effects in contrast to GlyT2 inhibitors reported by others.
前列腺癌骨痛(PCIBP)的病理生物学由炎症和神经病理性成分共同构成。在这里,我们使用 PCIBP 的大鼠模型来评估甘氨酸转运蛋白 2(GlyT2)抑制剂(N-(6-(1,3-二羟基-2-丙基)氨基)-2-(二甲基氨基)吡啶-3-基)-3,5-二甲氧基-4-(4-(三氟甲基)苯氧基)苯甲酰胺)相对于两种临床可用的辅助药物(即普瑞巴林和度洛西汀)的镇痛疗效,这些药物被推荐用于缓解神经病理性疼痛。
将大鼠前列腺癌细胞(AT3B)注入左侧胫骨,在雄性 Wistar Han 大鼠中诱导 PCIBP。假手术大鼠接受热灭活的 AT3B 细胞的 ITI。用 von Frey 纤维评估对侧后爪完全发展为机械性痛觉过敏的 PCIBP 大鼠,单次口服(p.o.)给予甘氨酸转运蛋白 2 抑制剂(3-30mg/kg)、普瑞巴林(3-100mg/kg)、度洛西汀(3-100mg/kg)或载体。在个体动物给药前和给药后 3 小时的预定时间,立即测定同侧(受伤侧)和对侧后爪的基础爪退缩阈值(PWTs)。
在测试剂量下,甘氨酸转运蛋白 2 抑制剂(3-30mg/kg)单次口服推注在 PCIBP 大鼠的同侧后爪中引起部分疼痛缓解,而没有明显的行为副作用。相比之下,普瑞巴林 10-100mg/kg 单次口服推注剂量依赖性地完全缓解机械性痛觉过敏。相比之下,度洛西汀的单次口服推注剂量高达 100mg/kg 缺乏疗效。
与其他人报告的甘氨酸转运蛋白 2 抑制剂相比,这种甘氨酸转运蛋白 2 抑制剂的口服给药在 PCIBP 大鼠中引起部分疼痛缓解,并且不会引起中枢神经系统副作用。
