首页> 外文期刊>Frontiers in Neuropharmacology >Prolonged Withdrawal From Escalated Oxycodone Is Associated With Increased Expression of Glutamate Receptors in the Rat Hippocampus
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Prolonged Withdrawal From Escalated Oxycodone Is Associated With Increased Expression of Glutamate Receptors in the Rat Hippocampus

机译:升级的羟考酮延长戒断与大鼠海马谷氨酸受体的表达增加有关

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People suffering from opioid use disorder (OUD) exhibit cognitive dysfunctions. Here, we investigated potential changes in the expression of glutamate receptors in rat hippocampi at 2 h and 31 days after the last session of oxycodone self-administration (SA). RNA extracted from the hippocampus was used in quantitative polymerase chain reaction analyses. Rats, given long-access (9 h per day) to oxycodone (LgA), took significantly more drug than rats exposed to short-access (3 h per day) (ShA). In addition, LgA rats could be further divided into higher oxycodone taking (LgA-H) or lower oxycodone taking (LgA-L) groups, based on a cut-off of 50 infusions per day. LgA rats, but not ShA, rats exhibited incubation of oxycodone craving. In addition, LgA rats showed increased mRNA expression of GluA1-3 and GluN2a-c subunits as well as Grm3, Grm5, Grm6, and Grm8 subtypes of glutamate receptors after 31 days but not after 2 h of stopping the SA experiment. Changes in GluA1-3, Grm6, and Grm8 mRNA levels also correlated with increased lever pressing (incubation) after long periods of withdrawal from oxycodone. More studies are needed to elucidate the molecular mechanisms involved in altering the expression of these receptors during withdrawal from oxycodone and/or incubation of drug seeking.
机译:患有阿片类药物使用障碍(OUD)的人表现出认知功能障碍。在这里,我们研究了在羟考酮自我给药(SA)最后一次会议后2小时和31天在大鼠海马中谷氨酸受体表达的潜在变化。从海马中提取的RNA用于定量聚合酶链反应分析。对羟考酮(LGA)的长期访问(每天9小时)进行大鼠比暴露于短途近期(每天3小时)(SHA)的大鼠显着增加药物。此外,基于每天50个输注的截止,LGA大鼠可以进一步分为高于羟考酮或降低羟考酮(LGA-L)或降低羟氢酮(LGA-L)组。 LGA大鼠,但不是SHA,大鼠表现出辛酮渴望的孵育。此外,LGA大鼠在31天后显示Glua1-3和Glun2A-C亚基的MRNA表达增加,GLUA1-3和GLUN2A-C亚基以及GRM3,GRM5,GRM6和GRM8亚籽型,但在2小时后停止SA实验后。 Glua1-3,GRM6和GRM8 mRNA水平的变化也与在从羟考酮的长时间戒断后的杠杆压迫(孵育)增加。需要更多的研究来阐明在从羟考酮和/或药物培养中撤离期间改变这些受体表达的分子机制。

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