一种新型的口服生物可利用的孤啡肽受体拮抗剂LY2940094可降低动物模型中的乙醇自我给药量和对乙醇的觅求行为。
A Novel, Orally Bioavailable Nociceptin Receptor Antagonist, LY2940094, Reduces Ethanol Self-Administration and Ethanol Seeking in Animal Models.
作者信息
Rorick-Kehn Linda M, Ciccocioppo Roberto, Wong Conrad J, Witkin Jeffrey M, Martinez-Grau Maria A, Stopponi Serena, Adams Benjamin L, Katner Jason S, Perry Kenneth W, Toledo Miguel A, Diaz Nuria, Lafuente Celia, Jiménez Alma, Benito Ana, Pedregal Concepción, Weiss Friedbert, Statnick Michael A
机构信息
Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, Indiana.
School of Pharmacy, Pharmacology Unit, University of Camerino, Camerino, Italy.
出版信息
Alcohol Clin Exp Res. 2016 May;40(5):945-54. doi: 10.1111/acer.13052. Epub 2016 Apr 16.
BACKGROUND
The nociceptin/orphanin-FQ (or opioid receptor-like [ORL1]) receptor (NOP) is localized in the mesolimbic reward pathway and has been suggested to play a role in feeding, mood, stress, and addiction. Since its deorphanization in 1995, there has been a clear dichotomy in the literature regarding whether an agonist or antagonist would provide therapeutic benefit. Specifically, the literature reports indicate that NOP receptor antagonists produce efficacy in animal models of hyperphagia and antidepressant-like activity, whereas NOP agonists produce anxiolytic-like effects and dampen reward/addiction behaviors including ethanol consumption.
METHODS
We characterize here the potent, orally bioavailable NOP antagonist, LY2940094, in rodent models of ethanol consumption, including ethanol self-administration, progressive ratio operant self-administration, stress-induced reinstatement of ethanol seeking, and in vivo microdialysis in the nucleus accumbens.
RESULTS
LY2940094 dose dependently reduced homecage ethanol self-administration in Indiana alcohol-preferring (P) and Marchigian Sardinian alcohol-preferring (msP) rats, without affecting food/water intake or locomotor activity. Reduced ethanol intake in P rats did not show significant tolerance over 4 days of subchronic dosing. LY2940094 attenuated progressive ratio operant responding and break points for ethanol in P rats. Moreover, stress-induced reinstatement of ethanol seeking in msP rats was completely blocked by LY2940094. Furthermore, LY2940094 blocked ethanol-stimulated dopamine release in response to ethanol challenge (1.1 g/kg, intraperitoneally).
CONCLUSIONS
Our findings demonstrate for the first time that blockade of NOP receptors attenuates ethanol self-administration and ethanol-motivated behaviors, stress-induced ethanol seeking, and ethanol-induced stimulation of brain reward pathways in lines of rats that exhibit excessive ethanol consumption. Results suggest that LY2940094 may have potential therapeutic utility in treating alcohol addiction.
背景
痛敏肽/孤啡肽FQ(或阿片样受体1 [ORL1])受体(NOP)定位于中脑边缘奖赏通路,且已表明其在进食、情绪、应激和成瘾中发挥作用。自1995年其被鉴定以来,关于激动剂或拮抗剂是否会带来治疗益处,文献中存在明显的分歧。具体而言,文献报道表明NOP受体拮抗剂在动物多食模型和类抗抑郁活性中产生疗效,而NOP激动剂产生类抗焦虑作用并抑制奖赏/成瘾行为,包括乙醇消耗。
方法
我们在此对强效的、口服生物可利用的NOP拮抗剂LY2940094在乙醇消耗的啮齿动物模型中进行表征,包括乙醇自我给药、渐进比率操作性自我给药、应激诱导的乙醇寻求恢复以及伏隔核的体内微透析。
结果
LY2940094剂量依赖性地减少了印第安纳嗜酒(P)大鼠和马尔基安撒丁岛嗜酒(msP)大鼠在笼内的乙醇自我给药,而不影响食物/水摄入或运动活性。P大鼠中乙醇摄入量的减少在亚慢性给药4天期间未显示出明显的耐受性。LY2940094减弱了P大鼠中乙醇的渐进比率操作性反应和断点。此外,LY2940094完全阻断了msP大鼠中应激诱导的乙醇寻求恢复。此外,LY2940094阻断了乙醇激发(1.1 g/kg,腹腔注射)引起的乙醇刺激的多巴胺释放。
结论
我们的研究结果首次证明,在表现出过量乙醇消耗的大鼠品系中,阻断NOP受体可减弱乙醇自我给药和乙醇驱动行为、应激诱导的乙醇寻求以及乙醇诱导的脑奖赏通路刺激。结果表明LY2940094在治疗酒精成瘾方面可能具有潜在的治疗效用。
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