偏向性μ阿片受体激动剂TRV130(oliceridine)急性和重复给药对啮齿动物抗伤害感受、胃肠功能及滥用可能性指标的影响
Effects of acute and repeated treatment with the biased mu opioid receptor agonist TRV130 (oliceridine) on measures of antinociception, gastrointestinal function, and abuse liability in rodents.
作者信息
Altarifi Ahmad A, David Bethany, Muchhala Karan H, Blough Bruce E, Akbarali Hamid, Negus S Stevens
机构信息
1 Faculty of Medicine, Jordan University of Science and Technology, Irbid, Jordan.
2 Department of Pharmacology and Toxicology, Virginia Commonwealth University, Richmond, VA, USA.
出版信息
J Psychopharmacol. 2017 Jun;31(6):730-739. doi: 10.1177/0269881116689257. Epub 2017 Feb 1.
RATIONALE
TRV130 (oliceridine; N-[(3-methoxythiophen-2-yl)methyl]-2-[(9 R)-9-pyridin-2-yl-6-oxaspiro[4.5]decan-9-yl]ethanamine) is a novel mu opioid receptor (MOR) agonist that preferentially activates G-protein versus β-arrestin signaling pathways coupled to MORs. Prevailing evidence suggests that TRV130 and other G-protein-biased MOR agonists may produce therapeutic analgesic effects with reduced adverse effects compared to existing MOR agonists.
OBJECTIVES
This study compared the effects of acute and repeated TRV130 administration on measures of antinociception, gastrointestinal function, and abuse liability in rodents. We hypothesized that TRV130 would produce robust and sustained antinociception and abuse-related effects during repeated treatment, but that tolerance would develop to gastrointestinal inhibition.
METHODS
Antinociception was assessed using a warm-water tail-withdrawal procedure in mice. Gastrointestinal function was assessed in mice using an in vivo measure of fecal output and in vitro assays of colonic propulsion and of colon and ileum circular muscle contraction. Abuse liability was assessed in rats using an intracranial self-stimulation (ICSS) procedure. (+)-TRV130 was administered with acute and repeated dosing regimens, and (-)-TRV130 was also examined in the ICSS procedure to assess stereoselectivity.
RESULTS
Acute (+)-TRV130 treatment produced robust antinociception, complete inhibition of gastrointestinal function, and weak abuse-related effects. Repeated (+)-TRV130 treatment failed to produce tolerance to antinociception or gastrointestinal inhibition, and abuse-related effects were enhanced by repeated treatment. Effects of acute and repeated (+)-TRV130 in these procedures resemble effects of morphine, with the exception that TRV130 antinociception was more resistant to tolerance. (-)-TRV130 was inactive.
CONCLUSIONS
These results suggest that TRV130 retains undesirable constipating and abuse-related effects during repeated treatment despite its bias for G-protein signaling.
原理
TRV130(oliceridine;N-[(3-甲氧基噻吩-2-基)甲基]-2-[(9R)-9-吡啶-2-基-6-氧杂螺[4.5]癸烷-9-基]乙胺)是一种新型的μ阿片受体(MOR)激动剂,与MOR偶联时,它优先激活G蛋白而非β-抑制蛋白信号通路。现有证据表明,与现有的MOR激动剂相比,TRV130和其他偏向G蛋白的MOR激动剂可能产生治疗性镇痛作用,且副作用减少。
目的
本研究比较了急性和重复给予TRV130对啮齿动物的镇痛、胃肠功能及滥用倾向指标的影响。我们假设,TRV130在重复治疗期间会产生强大且持续的镇痛及与滥用相关的效应,但对胃肠抑制会产生耐受性。
方法
采用温水甩尾法评估小鼠的镇痛作用。通过体内粪便排出量测量以及结肠推进、结肠和回肠环行肌收缩的体外试验评估小鼠的胃肠功能。采用颅内自我刺激(ICSS)程序评估大鼠的滥用倾向。急性和重复给药方案均给予(+)-TRV130,在ICSS程序中还检测了(-)-TRV130以评估立体选择性。
结果
急性给予(+)-TRV130可产生强大的镇痛作用,完全抑制胃肠功能,并产生较弱的与滥用相关的效应。重复给予(+)-TRV130未能产生镇痛耐受性或胃肠抑制耐受性,且重复治疗增强了与滥用相关的效应。急性和重复给予(+)-TRV130在这些程序中的效应与吗啡相似,不同之处在于TRV130的镇痛作用更不易产生耐受性。(-)-TRV130无活性。
结论
这些结果表明,尽管TRV130偏向G蛋白信号传导,但在重复治疗期间仍保留不良的便秘及与滥用相关的效应。
Zotero 插件