School of Pharmacy, Federal University of Bahia, 40.170-115, Salvador, BA, Brazil.
Department of Pharmaceutical Sciences, Federal University of Paraíba, 58.050-585, João Pessoa, PB, Brazil.
J Ethnopharmacol. 2024 Apr 6;323:117710. doi: 10.1016/j.jep.2024.117710. Epub 2024 Jan 4.
Ayahuasca (AYA) is a psychedelic brew used in religious ceremonies. It is broadly used as a sacred medicine for treating several ailments, including pain of various origins.
To investigate the antinociceptive effects of AYA and its mechanisms in preclinical models of acute and chronic pain in mice, in particular during experimental neuropathy.
The antinociceptive effects of AYA administered orally were assessed in the following models of pain: formalin test, Complete Freund's Adjuvant (CFA)-induced inflammation, tail flick test, and partial sciatic nerve ligation model of neuropathic pain. Antagonism assays and Fos immunohistochemistry in the brain were performed. AYA-induced toxicity was investigated. AYA was chemically characterized. The antinociceptive effect of harmine, the major component present in AYA, was investigated.
AYA (24-3000 μL/kg) dose-dependently reduced formalin-induced pain-like behaviors and CFA-induced mechanical allodynia but did not affect CFA-induced paw edema or tail flick latency. During experimental neuropathy, single treatments with AYA (24-3000 μL/kg) reduced mechanical allodynia; daily treatments once or twice a day for 14 days promoted consistent and sustained antinociception. The antinociceptive effect of AYA (600 μL/kg) was reverted by bicuculline (1 mg/kg) and methysergide (5 mg/kg), but not by naloxone (5 mg/kg), phaclofen (2 mg/kg), and rimonabant (10 mg/kg), suggesting the roles of GABA and serotonergic receptors. AYA increased Fos expression in the ventrolateral periaqueductal gray and nucleus raphe magnus after 1 h, but not after 6 h or 14 days of daily treatments. AYA (600 μL/kg) twice a day for 14 days did not alter mice's motor function, spontaneous locomotion, body weight, food and water intake, hematological, biochemical, and histopathological parameters. Harmine (3.5 mg/kg) promoted consistent antinociception during experimental neuropathy.
AYA promotes consistent antinociceptive effects in different mouse models of pain without inducing detectable toxic effects. Harmine is at least partially accountable for the antinociceptive properties of AYA.
阿育吠陀(AYA)是一种用于宗教仪式的迷幻草药。它被广泛用作治疗各种疾病的神圣药物,包括各种来源的疼痛。
在急性和慢性疼痛的小鼠临床前模型中,特别是在实验性神经病变期间,研究 AYA 的抗伤害作用及其机制。
通过以下疼痛模型评估口服 AYA 的抗伤害作用:福马林测试、完全弗氏佐剂(CFA)诱导的炎症、尾巴拍打测试和部分坐骨神经结扎神经病理性疼痛模型。进行了拮抗试验和脑中 Fos 免疫组织化学研究。研究了 AYA 诱导的毒性。对 AYA 进行了化学表征。研究了 AYA 中主要成分哈明的抗伤害作用。
AYA(24-3000μL/kg)剂量依赖性地减少福尔马林诱导的疼痛样行为和 CFA 诱导的机械性痛觉过敏,但不影响 CFA 诱导的足肿胀或尾巴拍打潜伏期。在实验性神经病变期间,单次给予 AYA(24-3000μL/kg)可减轻机械性痛觉过敏;每日治疗一次或两次,共 14 天,可促进持续和持续的镇痛作用。600μL/kg AYA 的镇痛作用被毒扁豆碱(1mg/kg)和甲硫丝氨酸(5mg/kg)逆转,但不受纳洛酮(5mg/kg)、phaclofen(2mg/kg)和利莫那班(10mg/kg)的影响,提示 GABA 和 5-羟色胺能受体的作用。AYA 在 1 小时后增加了腹外侧导水管周围灰质和中缝大核中 Fos 的表达,但在 6 小时或 14 天后的每日治疗中没有增加。AYA(600μL/kg)每日两次,共 14 天,不改变小鼠的运动功能、自发运动、体重、食物和水的摄入、血液学、生化和组织病理学参数。哈明(3.5mg/kg)在实验性神经病变期间促进了一致的镇痛作用。
AYA 在不同的小鼠疼痛模型中促进一致的镇痛作用,而不会引起可检测的毒性作用。哈明至少部分解释了 AYA 的镇痛特性。
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