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首页> 外文期刊>Addiction biology >Cocaine-elicited imbalances in ventromedial prefrontal cortex Homer1 versus Homer2 expression: Implications for relapse
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Cocaine-elicited imbalances in ventromedial prefrontal cortex Homer1 versus Homer2 expression: Implications for relapse

机译:可卡因引起腹侧前额叶皮层Homer1与Homer2表达的失衡:对复发的影响

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Withdrawal from a history of extended access to self-administered cocaine produces a time-dependent intensification of drug seeking, which might relate to a cocaine-induced imbalance in the relative expression of constitutively expressed Homer1 versus Homer2 isoforms within the ventromedial aspect of the prefrontal cortex (vmPFC). Thus, we employed immunoblotting to examine the relation between cue-reinforced lever pressing at 3- versus 30-day withdrawal from a 10-day history of extended access (6 hours/day) to intravenous cocaine (0.25mg/infusion) or saline (Sal6h), and the expression of Homer1b/c and Homer2a/b within the vmPFC versus the more dorsomedial aspect of this structure (dmPFC). Behavioral studies employed adeno-associated virus (AAV) vectors to reverse cocaine-elicited changes in the relative expression of Homer1 versus Homer2 isoforms and tested animals for cocaine prime-, and cue-induced responding following extinction training. Cocaine self-administration elevated both Homer1b/c and Homer2a/b levels within the vmPFC at 3-day withdrawal, and the rise in Homer2a/b persisted for at least 30 days. dmPFC Homer levels did not change as a function of self-administration history. Reversing the relative increase in Homer2 versus Homer1 expression via Homer1c overexpression or Homer2b knockdown failed to influence cue-reinforced lever pressing when animals were tested in a drug-free state, but both AAV treatments prevented cocaine-primed reinstatement of lever-pressing behavior. These data suggest that a cocaine-elicited imbalance in the relative expression of constitutively expressed Homer2 versus Homer1 within the vmPFC is necessary for the capacity of cocaine to reinstate drug-seeking behavior, posing drug-induced changes in vmPFC Homer expression as a molecular trigger contributing to drug-elicited relapse. Herein, we demonstrated by immunoblotting that withdrawal from a history of heavy cocaine-taking resulted in a time-dependent imbalance in the relative expression of Homer1b/c and Homer2a/b isoforms within the ventromedial prefrontal cortex (vmPFC) of rats. Using a virus-mediated transgene delivery strategy, we showed that reversing this imbalance by elevating Homer1c or reducing Homer2b within vmPFC prevented the manifestion of cocaine-primed reinstatement of drug-seeking, following extinction.
机译:从长期接触自我管理的可卡因的历史中退出,会导致时间依赖性的药物寻找加剧,这可能与可卡因诱导的前额叶皮层腹侧组成性表达的Homer1和Homer2亚型的相对表达不平衡有关。 (vmPFC)。因此,我们采用免疫印迹法研究了从10天的延长使用时间(6小时/天)到静脉注射可卡因(0.25mg /滴注)或生理盐水(3天或30天撤药)后,提示增强的杠杆按压在3天和30天之间的关系。 Sal6h),以及vmPFC中Homer1b / c和Homer2a / b的表达与该结构的更靠背的方面(dmPFC)相比。行为研究采用腺相关病毒(AAV)载体逆转可卡因引起的Homer1与Homer2同种型相对表达的变化,并测试了灭绝训练后可卡因引发和提示诱导的反应的动物。停用3天后,可卡因自我管理同时升高了vmPFC中的Homer1b / c和Homer2a / b水平,而Homer2a / b的升高至少持续了30天。 dmPFC Homer的级别没有根据自我管理历史记录而变化。当在无药物状态下对动物进行测试时,通过Homer1c过表达或Homer2b敲低来逆转Homer2与Homer1表达的相对增加,不会影响提示增强的杠杆按压,但是两种AAV处理均阻止了可卡因引发的杠杆按压行为的恢复。这些数据表明,可卡因引起的vmPFC中组成型表达的Homer2与Homer1相对表达的失衡对于可卡因恢复寻药行为的能力是必要的,从而将药物诱导的vmPFC Homer表达的变化视为分子触发因素药物引起的复发。在这里,我们通过免疫印迹法证明,从服用大量可卡因的历史中撤离会导致大鼠腹侧前额叶皮层(vmPFC)中Homer1b / c和Homer2a / b同种型的相对表达出现时间依赖性失衡。使用病毒介导的转基因传递策略,我们证明了通过升高vmPFC中的Homer1c或减少Homer2b来逆转这种失衡现象,从而防止了可卡因引发的灭绝后药物寻找的恢复。

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