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一种新型吗啡灌胃法建立大鼠阿片类药物依赖模型。

A Novel Morphine Drinking Model of Opioid Dependence in Rats.

机构信息

Center for Regenerative Medicine, Faculty of Medicine Clínica Alemana, Universidad del Desarrollo, Santiago 7610658, Chile.

Molecular and Clinical Pharmacology Program, Institute of Biomedical Science, Faculty of Medicine, Universidad de Chile, Santiago 8380453, Chile.

出版信息

Int J Mol Sci. 2022 Mar 31;23(7):3874. doi: 10.3390/ijms23073874.

DOI:10.3390/ijms23073874
PMID:35409269
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8999131/
Abstract

An animal model of voluntary oral morphine consumption would allow for a pre-clinical evaluation of new treatments aimed at reducing opioid intake in humans. However, the main limitation of oral morphine consumption in rodents is its bitter taste, which is strongly aversive. Taste aversion is often overcome by the use of adulterants, such as sweeteners, to conceal morphine taste or bitterants in the alternative bottle to equalize aversion. However, the adulterants' presence is the cause for consumption choice and, upon removal, the preference for morphine is not preserved. Thus, current animal models are not suitable to study treatments aimed at reducing consumption elicited by morphine itself. Since taste preference is a learned behavior, just-weaned rats were trained to accept a bitter taste, adding the bitterant quinine to their drinking water for one week. The latter was followed by allowing the choice of quinine or morphine (0.15 mg/mL) solutions for two weeks. Then, quinine was removed, and the preference for morphine against water was evaluated. Using this paradigm, we show that rats highly preferred the consumption of morphine over water, reaching a voluntary morphine intake of 15 mg/kg/day. Morphine consumption led to significant analgesia and hyperlocomotion, and to a marked deprivation syndrome following the administration of the opioid antagonist naloxone. Voluntary morphine consumption was also shown to generate brain oxidative stress and neuroinflammation, signs associated with opioid dependence development. We present a robust two-bottle choice animal model of oral morphine self-administration for the evaluation of therapeutic interventions for the treatment of morphine dependence.

摘要

一种自愿口服吗啡消费的动物模型将允许对旨在减少人类阿片类药物摄入的新治疗方法进行临床前评估。然而,啮齿动物口服吗啡消费的主要限制是其苦味,这是强烈的厌恶感。为了掩盖吗啡的味道,通常使用甜味剂等添加剂来克服味觉厌恶,或者在替代瓶中添加苦味剂来平衡厌恶感。然而,添加剂的存在是导致消费选择的原因,一旦去除,对吗啡的偏好就不会保留。因此,目前的动物模型不适合研究旨在减少吗啡本身引起的消费的治疗方法。由于味觉偏好是一种习得行为,刚断奶的大鼠被训练接受苦味,在饮用水中添加苦味剂奎宁一周。随后,允许大鼠选择奎宁或吗啡(0.15mg/mL)溶液两周。然后,去除奎宁,并评估大鼠对吗啡与水的偏好。使用这种范式,我们表明大鼠非常喜欢消耗吗啡而不是水,达到每天 15mg/kg 的自愿吗啡摄入量。吗啡消耗导致明显的镇痛和过度活跃,并在给予阿片拮抗剂纳洛酮后出现明显的剥夺综合征。自愿吗啡消耗也被证明会导致大脑氧化应激和神经炎症,这些迹象与阿片类药物依赖的发展有关。我们提出了一种可靠的口服吗啡自我给药的双瓶选择动物模型,用于评估治疗干预吗啡依赖的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2983/8999131/20dcd84f94a4/ijms-23-03874-g008.jpg
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