Opioid-Induced Inter-regional Dysconnectivity Correlates with Analgesia in Awake Mouse Brains

Jean-Charles Mariani, Samual Diebolt, Laurianne Beynac, Renata Santos, Stefan Schulz, Thomas Deffieux, Mickael Tanter, Zsolt LENKEI, Andrea Kliewer
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Abstract

The mu-opioid receptor (MOP) is crucial for both the therapeutic and addictive effects of opioids. Using a multimodal experimental approach, here we combined awake functional ultrasound (fUS) imaging with behavioral and molecular assessments, to examine opioid-induced changes in brain activation and functional connectivity (FC). Morphine, fentanyl, and methadone induce significant dose- and time-dependent reorganization of brain perfusion, oscillations and FC in awake mice. Notably, opioids induce a transient, region-specific hyperperfusion, followed by a consistent MOP-specific dysconnectivity marked by decreased FC of the somatosensory cortex to hippocampal and thalamic regions, alongside increased subcortical and intra-cortical FC. These FC changes temporally correlate with generalized brain MOP activation and analgesia, but not with hypermobility and respiratory depression, suggesting a reorganization of inter-regional FC as a key opioid effect.
阿片类药物诱导的区域间连接失调与清醒小鼠大脑的镇痛有关
μ阿片受体(MOP)对阿片类药物的治疗和成瘾作用至关重要。在这里,我们采用多模式实验方法,将清醒状态下的功能超声成像(fUS)与行为和分子评估相结合,研究阿片类药物诱导的大脑激活和功能连接(FC)变化。吗啡、芬太尼和美沙酮可诱导清醒小鼠大脑灌注、振荡和功能连接发生显著的剂量和时间依赖性重组。值得注意的是,阿片类药物会诱导一过性、区域特异性的高灌注,随后出现一致的澳门巴黎人娱乐官网特异性连接障碍,表现为躯体感觉皮层与海马和丘脑区域的FC下降,同时皮层下和皮层内的FC增加。这些FC变化在时间上与广泛的脑澳门巴黎人娱乐官网激活和镇痛相关,但与过度运动和呼吸抑制无关,这表明区域间FC重组是阿片类药物的关键效应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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