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大鼠酒精戒断综合征期间,导水管周围灰质中κ阿片受体的药理超敏反应。

Pharmacologic hyperreactivity of kappa opioid receptors in periaqueductal gray matter during alcohol withdrawal syndrome in rats.

机构信息

Departamento de Fisiología Y Farmacología, Centro de Ciencias Básicas, Universidad Autónoma de Aguascalientes, 20131, Aguascalientes, Ags, Mexico.

Laboratorio de Neuropsicofarmacología, Facultad de Psicología, Universidad Nacional Autónoma de México, 04510, Mexico City, Mexico.

出版信息

Pharmacol Rep. 2023 Oct;75(5):1299-1308. doi: 10.1007/s43440-023-00522-z. Epub 2023 Sep 2.

DOI:10.1007/s43440-023-00522-z
PMID:37658980
Abstract

BACKGROUND

Periaqueductal gray matter (PAG) is a brain region rich in kappa-opioid receptors (KOR). KOR in PAG mediates behavioral responses related to pain integration, and panic response, among others. Its participation in the addiction phenomena has been poorly studied. Hence, this preliminary study explored the pharmacological effects of KOR stimulation/blockade in dorsal-PAG (D-PAG) during alcohol withdrawal on anxiety-type behaviors and alcohol intake/preference.

METHODS

Juvenile male Wistar rats were unexposed (A-naïve group) or exposed to alcohol for 5 weeks and then restricted (A-withdrawal group). Posteriorly, animals received intra D-PAG injections of vehicle (10% DMSO), salvinorin A (SAL-A; a selective KOR agonist), or 2-Methyl-N-((2'-(pyrrolidin-1-ylsulfonyl)biphenyl-4-yl)methyl)propan-1-amine (PF-04455242; a highly selective KOR-antagonist). Subsequently, the defensive burying behavior (DBB) and alcohol intake/preference paradigms were evaluated.

RESULTS

SAL-A markedly increased burying time, the height of bedding, and alcohol consumption/preference in A-withdrawal, while slightly increased the height of bedding in A-näive rats. PF-04455242 decreased both burying and immobility duration, whereas increases latency to burying, frequency of rearing, and the number of stretches attempts with no action on alcohol intake/preference in A-withdrawal rats.

CONCLUSIONS

In general, stimulation/blockade of KOR in A-withdrawal animals exert higher responses compared to A-naïve ones. SAL-A produced anxiety-like behaviors and increased alcohol consumption/preference, especially/solely in the alcohol-withdrawal condition, while PF-04455242 augmented exploration with no effects on alcohol intake/preference. Our findings suggest a possible pharmacologic hyperreactivity of the KOR in PAG during alcohol withdrawal.

摘要

背景

导水管周围灰质(periaqueductal gray matter,PAG)富含κ-阿片受体(kappa-opioid receptor,KOR)。PAG 中的 KOR 介导与疼痛整合、惊恐反应等相关的行为反应。其在成瘾现象中的参与尚未得到充分研究。因此,本初步研究探索了酒精戒断期间背侧 PAG(dorsal-PAG,D-PAG)中 KOR 刺激/阻断对焦虑样行为和酒精摄入/偏好的药理学影响。

方法

雄性幼 Wistar 大鼠未暴露(A-未暴露组)或暴露于酒精 5 周,然后限制(A-戒断组)。随后,动物接受 D-PAG 内注射载体(10% DMSO)、沙利洛芬 A(SAL-A;选择性 KOR 激动剂)或 2-甲基-N-((2'-(吡咯烷-1-基磺酰基)联苯-4-基)甲基)丙-1-胺(PF-04455242;高度选择性 KOR 拮抗剂)。随后,评估防御性掩埋行为(defensive burying behavior,DBB)和酒精摄入/偏好范式。

结果

SAL-A 显著增加 A-戒断大鼠的掩埋时间、垫料高度和酒精摄入/偏好,而略微增加 A-未暴露大鼠的垫料高度。PF-04455242 降低掩埋和不动时间,而增加掩埋潜伏期、后肢抬高频率和伸展尝试次数,对 A-戒断大鼠的酒精摄入/偏好无作用。

结论

一般来说,KOR 在 A-戒断动物中的刺激/阻断比 A-未暴露动物产生更高的反应。SAL-A 产生焦虑样行为并增加酒精摄入/偏好,特别是/仅在酒精戒断条件下,而 PF-04455242 增加探索但对酒精摄入/偏好无影响。我们的发现表明,酒精戒断期间 PAG 中的 KOR 可能存在药理学超反应性。

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Medullary kappa-opioid receptor neurons inhibit pain and itch through a descending circuit.延髓κ阿片受体神经元通过下行环路抑制痛觉和瘙痒。
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