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新型内吗啡肽类似物的鉴别刺激和低滥用倾向作用表明其可能成为治疗阿片类药物使用障碍的一种手段。

Discriminative Stimulus and Low Abuse Liability Effects of Novel Endomorphin Analogs Suggest a Potential Treatment Indication for Opioid Use Disorder.

机构信息

Southeast Louisiana Veterans Health Care System (J.E.Z.), Departments of Medicine (J.E.Z.), Neuroscience (M.R.N., M.L., C.C., L.A., J.V., J.E.Z.), and Pharmacology (J.E.Z.), Tulane University School of Medicine, New Orleans, Louisiana.

Southeast Louisiana Veterans Health Care System (J.E.Z.), Departments of Medicine (J.E.Z.), Neuroscience (M.R.N., M.L., C.C., L.A., J.V., J.E.Z.), and Pharmacology (J.E.Z.), Tulane University School of Medicine, New Orleans, Louisiana

出版信息

J Pharmacol Exp Ther. 2019 Sep;370(3):369-379. doi: 10.1124/jpet.118.253013. Epub 2019 Jun 18.

Abstract

Opioid dependence can be difficult to manage using existing pharmacotherapies. A long-acting opioid with low abuse liability that substitutes for a shorter-acting opioid may improve treatment of opioid use disorders (OUDs). We recently characterized an endomorphin (EM) analog (ZH853) that produced a longer duration of antinociception compared with morphine, but did not produce self-administration or several other adverse effects preclinically. Here, we further characterized ZH853 in tests of antinociception, abuse liability, and drug discrimination. A conditioned place preference (CPP) procedure, that included a locomotor activity assessment, was used to test abuse liability in rats. Subsequently, dopamine (DA) cell-somas located in the ventral tegmental area (VTA) from these rats were assessed by size using immunohistochemistry and Stereo Investigator software. A hot-plate antinociception test in male and female mice confirmed central penetration. Morphine-substitution effects of several EM analogs (ZH850, ZH831, and ZH853) were tested in a drug discrimination (DD) procedure in rats. Morphine produced dose-dependent CPP and locomotor sensitization and reduced the size of DA cell somas in VTA, whereas ZH853 did not produce any of these effects relative to control. The antinociceptive effects of ZH853 were -receptor selective since -funaltrexamine antagonized these effects. Rats responded on a morphine-trained lever when injected with ZH831 and ZH853 during DD experiments. The favorable morphine-substitution effects of these EM analogs relative to their low abuse liability indicate promising novel compounds that may improve treatment of OUD. SIGNIFICANCE STATEMENT: In this experiment, we investigated the preclinical effects of novel endomorphin analogs for use as substitution therapies for opioid use disorder, a problem that has contributed to an opioid overdose epidemic. Several endomorphin analogs substituted for morphine without producing adverse effects, including reward behaviors associated with abuse liability. These compounds have the potential to become important additional tools to treat opioid use disorders.

摘要

阿片类药物依赖使用现有药物治疗可能比较困难。一种长效、滥用风险低的阿片类药物,可替代短效阿片类药物,可能改善阿片类药物使用障碍(OUD)的治疗。我们最近研究了一种内吗啡肽(EM)类似物(ZH853),它产生的镇痛作用持续时间比吗啡长,但在临床前研究中没有产生自我给药或其他几种不良反应。在这里,我们进一步研究了 ZH853 在镇痛、滥用倾向和药物辨别方面的特性。在大鼠中使用条件性位置偏好(CPP)程序,包括运动活动评估,来测试滥用倾向。随后,通过免疫组织化学和 Stereo Investigator 软件评估这些大鼠腹侧被盖区(VTA)中的多巴胺(DA)细胞体的大小。在雄性和雌性小鼠中进行热板镇痛测试,以确认药物是否穿透中枢神经系统。在大鼠的药物辨别(DD)程序中,测试了几种 EM 类似物(ZH850、ZH831 和 ZH853)的吗啡替代作用。吗啡产生剂量依赖性 CPP 和运动敏化作用,并减少 VTA 中 DA 细胞体的大小,而 ZH853 与对照相比,不会产生任何这些作用。ZH853 的镇痛作用是 μ-受体选择性的,因为 -funaltrexamine 拮抗了这些作用。在 DD 实验中,当大鼠注射 ZH831 和 ZH853 时,它们会对吗啡训练的杠杆产生反应。这些 EM 类似物相对于其低滥用倾向的吗啡替代作用表明,这些类似物是很有前途的新型化合物,可能改善 OUD 的治疗效果。意义:在这项实验中,我们研究了新型内吗啡肽类似物作为阿片类药物使用障碍替代治疗的临床前作用,阿片类药物使用障碍导致了阿片类药物过量流行。几种内吗啡肽类似物替代了吗啡,而没有产生不良反应,包括与滥用倾向相关的奖励行为。这些化合物有可能成为治疗阿片类药物使用障碍的重要补充工具。

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