α-蒎烯对小鼠吗啡耐受性和依赖性的毒性和生物效应评估

IF 1 Q4 PHARMACOLOGY & PHARMACY Jundishapur Journal of Natural Pharmaceutical Products Pub Date : 2023-11-27 DOI:10.5812/jjnpp-141534
Nasrin Nasrin Hajiabadi, Saeid Abbasi Maleki, Zahra Mousavi, P. Najafizadeh
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引用次数: 0

摘要

背景:研究表明,α-蒎烯与阿片能系统相互作用。研究目的本研究旨在探讨 α-蒎烯的毒性及其对小鼠吗啡耐受性和依赖性的影响。研究方法:分别采用第 423 号和第 407 号准则研究急性和亚慢性毒性。在亚慢性毒性分析中,动物在第 28 天被处死,并采集血液和组织样本。在诱导吗啡耐受性或依赖性后,在两个阶段中,动物分别接受静脉注射载体、地西泮(5 毫克/千克)和 α-蒎烯(3.125、6.25 和 12.5 毫克/千克)。在30分钟内记录戒断症状。结果显示只有急性剂量的α-蒎烯会导致动物死亡,但亚慢性剂量的α-蒎烯会导致小鼠大脑、肝脏和肾脏出现轻微病变。此外,雌性小鼠的谷丙转氨酶(ALT)、谷草转氨酶(AST)、谷草转氨酶(ALP)和谷草转氨酶(TG)水平升高(P < 0.05)。此外,α-蒎烯剂量为 6.25 和 12.5 毫克/千克(P < 0.001),只有高剂量(12.5 毫克/千克)(P < 0.001)可分别减少耐受期和依赖期的跳跃次数。在耐受阶段,腹泻(P < 0.001)、蠕动(P < 0.001)、饲养和攀爬(分别为 P < 0.05 和 P < 0.001)行为减少;在依赖阶段,梳理、攀爬和牙齿颤动行为减少(P < 0.001)。结论α-蒎烯的半数致死剂量低于2000毫克/千克,但其亚慢性剂量会引起轻微的组织毒性和生化变化。此外,α-蒎烯还能降低吗啡的耐受性和依赖性,经过免费试验后,α-蒎烯可能有助于治疗阿片类药物依赖。
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Assessment of Toxicity and Biological Effects of α-Pinene on Morphine Tolerance and Dependence in Mice
Background: Research shows that α-Pinene interacts with the opioidergic system. Objectives: This study aims to examine the toxicity and the effects of α-Pinene on morphine tolerance and dependence in mice. Methods: Guidelines No. 423 and No. 407 were used to investigate acute and sub-chronic toxicity, respectively. For sub-chronic toxicity analysis, the animals were sacrificed on day 28, and blood and tissue samples were collected. After inducing morphine tolerance or dependence, in both phases, animals received i.p. vehicle, diazepam (5 mg/kg), and α-Pinene (3.125, 6.25, and 12.5 mg/kg). Withdrawal signs were recorded for 30 minutes. Results: Only the acute dose of α-Pinene showed mortality in animals, but mild lesions were seen in the brain, liver, and kidneys in the mice receiving its subchronic dose. Moreover, ALT, AST, ALP, and TG levels increased (P < 0.05) in female mice. Besides, 6.25 and 12.5 mg/kg (P < 0.001) of α-Pinene and only its high dose (12.5 mg/kg) (P < 0.001) reduced the number of jumps in the tolerance and dependence phases, respectively. Diarrhea (P < 0.001), writhing (P < 0.001), rearing, and climbing (P < 0.05 and P < 0.001, respectively) behaviors decreased in the tolerance phase, and grooming, climbing, and teeth chattering declined in the dependence phase (P < 0.001). Conclusions: The LD50 of α-Pinene was lower than 2000 mg/kg, but its subchronic dose caused mild tissue toxicities and biochemical changes. Moreover, α-Pinene decreased morphine tolerance and dependence and possibly was useful for the treatment of opioid dependence after complimentary trials.
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