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外侧眶额皮层对恐惧调节和酒精消费的机制进行分区。

Lateral orbitofrontal cortex partitions mechanisms for fear regulation and alcohol consumption.

机构信息

Department of Psychology, Boston College, Chestnut Hill, Massachusetts, United States of America.

出版信息

PLoS One. 2018 Jun 1;13(6):e0198043. doi: 10.1371/journal.pone.0198043. eCollection 2018.

Abstract

Anxiety disorders and alcohol use disorder are highly comorbid, yet identifying neural dysfunction driving comorbidity has been challenging. Lateral orbitofrontal cortex (lOFC) dysfunction has been independently observed in each disorder. Here we tested the hypothesis that the lOFC is essential to partition mechanisms for fear regulation and alcohol consumption. Specifically, the capacity to regulate fear and the propensity to consume alcohol are unrelated when lOFC is intact, but become linked through lOFC dysfunction. Male Long Evans rats received bilateral, neurotoxic lOFC lesions or sham surgery. Fear regulation was determined by establishing discrimination to danger, uncertainty, and safety cues then shifting the shock probability of the uncertainty cue. Alcohol consumption was assessed through voluntary, intermittent access to 20% ethanol. The neurotoxic lesion approach ensured lOFC dysfunction spanned testing in fear regulation and alcohol consumption. LOFC-lesioned rats demonstrated maladaptive fear generalization during probability shifts, inverting normal prediction error assignment, and subsequently consumed more alcohol. Most novel, fear regulation and alcohol consumption were inextricably linked only in lOFC-lesioned rats: extreme fear regulation predicted excessive alcohol consumption. The results reveal the lOFC is essential to partition mechanisms for fear regulation and alcohol consumption and uncover a plausible source of neural dysfunction contributing to comorbid anxiety disorders and alcohol use disorder.

摘要

焦虑症和酒精使用障碍高度共病,但确定导致共病的神经功能障碍一直具有挑战性。外侧眶额皮层(lOFC)功能障碍在每种疾病中都有独立观察到。在这里,我们检验了这样一个假设,即 lOFC 对于区分恐惧调节和酒精消费的机制是必不可少的。具体来说,当 lOFC 完好无损时,调节恐惧的能力和饮酒的倾向是无关的,但通过 lOFC 功能障碍它们会联系在一起。雄性 Long Evans 大鼠接受双侧、神经毒性 lOFC 损伤或假手术。通过建立对危险、不确定性和安全线索的辨别来确定恐惧调节,然后改变不确定性线索的电击概率。通过自愿、间歇性地接触 20%乙醇来评估酒精消费。神经毒性损伤方法确保 lOFC 功能障碍贯穿于恐惧调节和酒精消费的测试中。lOFC 损伤大鼠在概率转移时表现出适应性不良的恐惧泛化,颠倒了正常的预测误差分配,随后消耗了更多的酒精。最具创新性的是,只有在 lOFC 损伤大鼠中,恐惧调节和酒精消费才紧密相关:极端的恐惧调节预示着过度饮酒。研究结果表明,lOFC 对于区分恐惧调节和酒精消费的机制是必不可少的,并揭示了导致共病焦虑症和酒精使用障碍的神经功能障碍的一个可能来源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3ab1/5983516/7292fb271c61/pone.0198043.g001.jpg

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