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吗啡耐受小鼠急性和慢性给予吗啡后血浆代谢特征的变化

Changes in Plasma Metabolic Signature upon Acute and Chronic Morphine Administration in Morphine-Tolerant Mice.

作者信息

Kutchy Naseer A, Palermo Amelia, Ma Rong, Li Zhong, Ulanov Alexandria, Callen Shannon, Siuzdak Gary, Roy Sabita, Buch Shilpa, Hu Guoku

机构信息

Department of Animal Sciences, Rutgers, The State University of New Jersey, New Brunswick, NJ 08901, USA.

Department of Pharmacology and Experimental Neuroscience, University of Nebraska Medical Center, Omaha, NE 68198, USA.

出版信息

Metabolites. 2023 Mar 16;13(3):434. doi: 10.3390/metabo13030434.

Abstract

Morphine administration causes system-level metabolic changes. Here, we show that morphine-tolerant mice exhibited distinct plasma metabolic signatures upon acute and chronic administration. We utilized a mouse model of morphine tolerance by exposing mice to increasing doses of the drug over 4 days. We collected plasma samples from mice undergoing acute or chronic morphine or saline injections and analyzed them using targeted GC-MS-based metabolomics to profile approximately 80 metabolites involved in the central carbon, amino acid, nucleotide, and lipid metabolism. Our findings reveal distinct alterations in plasma metabolite concentrations in response to acute or chronic morphine intake, and these changes were linked to the development of tolerance to morphine's analgesic effects. We identified several metabolites that had been differentially affected by acute versus chronic morphine use, suggesting that metabolic changes may be mitigated by prolonged exposure to the drug. Morphine-tolerant mice showed a restoration of amino acid and glycolytic metabolites. Additionally, we conducted reconstructed metabolic network analysis on the first 30 VIP-ranked metabolites from the PLSDA of the saline, acute, and morphine-tolerant mice groups, which uncovered four interaction networks involving the amino acid metabolism, the TCA cycle, the glutamine-phenylalanine-tyrosine pathway, and glycolysis. These pathways were responsible for the metabolic differences observed following distinct morphine administration regimens. Overall, this study provides a valuable resource for future investigations into the role of metabolites in morphine-induced analgesia and associated effects following acute or chronic use in mice.

摘要

吗啡给药会引起系统水平的代谢变化。在此,我们表明,急性和慢性给药后,吗啡耐受小鼠呈现出独特的血浆代谢特征。我们通过在4天内让小鼠接触递增剂量的药物,建立了吗啡耐受小鼠模型。我们从接受急性或慢性吗啡或生理盐水注射的小鼠身上采集血浆样本,并使用基于靶向气相色谱-质谱联用的代谢组学方法对其进行分析,以描绘大约80种参与中心碳、氨基酸、核苷酸和脂质代谢的代谢物。我们的研究结果揭示了急性或慢性吗啡摄入后血浆代谢物浓度的明显变化,这些变化与对吗啡镇痛作用的耐受性发展有关。我们鉴定出几种受急性与慢性吗啡使用影响存在差异的代谢物,这表明长期接触该药物可能会减轻代谢变化。吗啡耐受小鼠的氨基酸和糖酵解代谢物有所恢复。此外,我们对生理盐水组、急性吗啡组和吗啡耐受小鼠组的PLSDA分析中前30个VIP排名的代谢物进行了重建代谢网络分析,发现了四个相互作用网络,涉及氨基酸代谢、三羧酸循环、谷氨酰胺-苯丙氨酸-酪氨酸途径和糖酵解。这些途径导致了不同吗啡给药方案后观察到的代谢差异。总的来说,本研究为未来研究代谢物在小鼠急性或慢性使用吗啡诱导的镇痛及相关效应中的作用提供了宝贵资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f188/10053579/6813adc0263c/metabolites-13-00434-g001.jpg

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