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早年逆境会促进可卡因自我给药的习得,并诱发持续性快感缺失。

Early-life adversity facilitates acquisition of cocaine self-administration and induces persistent anhedonia.

作者信息

Bolton Jessica L, Ruiz Christina M, Rismanchi Neggy, Sanchez Gissell A, Castillo Erik, Huang Jeff, Cross Christopher, Baram Tallie Z, Mahler Stephen V

机构信息

Department of Anatomy & Neurobiology, University of California, Irvine, USA.

Department of Neurobiology & Behavior, University of California, Irvine, USA.

出版信息

Neurobiol Stress. 2018 Jan 12;8:57-67. doi: 10.1016/j.ynstr.2018.01.002. eCollection 2018 Feb.

Abstract

Early-life adversity increases the risk for emotional disorders such as depression and schizophrenia. Anhedonia, thought to be a core feature of these disorders, is provoked by our naturalistic rodent model of childhood adversity (i.e., rearing pups for one week in cages with limited bedding and nesting, LBN). Drug use and addiction are highly comorbid with psychiatric disorders featuring anhedonia, yet effects of LBN on drug-seeking behavior and the reward and stress-related circuits that underlie it remain unknown. Here we examined the effects of LBN on cocaine intake and seeking, using a battery of behavioral tests measuring distinct aspects of cocaine reward, and for comparison, chocolate intake. We also examined activation of neurons within the pleasure/reward and stress circuits following cocaine in LBN and control rats. Early-life adversity reduced spontaneous intake of palatable chocolate, extending prior reports of sucrose and social-play anhedonia. In a within-session cocaine behavioral economic test, LBN rats self-administered lower dosages of cocaine under low-effort conditions, consistent with a reduced hedonic set-point for cocaine, and potentially anhedonia. In contrast, cocaine demand elasticity was not consistently affected, indicating no major changes in motivation to maintain preferred cocaine blood levels. These changes were selective, as LBN did not cause an overt anxiety-like phenotype, nor did it affect sensitivity to self-administered cocaine dose, responding for cocaine under extinction conditions, cocaine- or cue-induced reinstatement of cocaine seeking, or locomotor response to acute cocaine. However, high Fos expression was seen after cocaine in both reward- and stress-related brain regions of LBN rats, including nucleus accumbens core, central amygdala, and lateral habenula. In contrast, hypothalamic orexin neuron activation after cocaine was significantly attenuated in LBN rats. Together, these findings demonstrate enduring effects of early-life adversity on both reward- and fear/anxiety-related neural circuits, as well as anhedonia-like reductions in consumption of natural and drug rewards.

摘要

早年逆境会增加患抑郁症和精神分裂症等情绪障碍的风险。快感缺失被认为是这些障碍的核心特征,我们的童年逆境自然主义啮齿动物模型(即在垫料和筑巢有限的笼子里饲养幼崽一周,LBN)会引发快感缺失。药物使用和成瘾与以快感缺失为特征的精神障碍高度共病,但LBN对药物寻求行为以及作为其基础的奖赏和应激相关回路的影响尚不清楚。在这里,我们使用一系列测量可卡因奖赏不同方面的行为测试,并以巧克力摄入量作比较,研究了LBN对可卡因摄入量和寻求行为的影响。我们还研究了LBN大鼠和对照大鼠在给予可卡因后,快感/奖赏和应激回路中神经元的激活情况。早年逆境减少了可口巧克力的自发摄入量,扩展了先前关于蔗糖和社交游戏快感缺失的报道。在一次可卡因行为经济学测试中,LBN大鼠在低努力条件下自我给药的可卡因剂量较低,这与可卡因享乐阈值降低一致,可能存在快感缺失。相比之下,可卡因需求弹性并未受到持续影响,表明维持首选可卡因血药浓度的动机没有重大变化。这些变化具有选择性,因为LBN既没有导致明显的焦虑样表型,也没有影响对自我给药可卡因剂量的敏感性、在消退条件下对可卡因的反应、可卡因或线索诱导的可卡因寻求恢复,或对急性可卡因的运动反应。然而,在LBN大鼠的奖赏和应激相关脑区,包括伏隔核核心、中央杏仁核和外侧缰核,给予可卡因后可见高Fos表达。相比之下,LBN大鼠给予可卡因后下丘脑食欲素神经元的激活明显减弱。总之,这些发现表明早年逆境对奖赏和恐惧/焦虑相关神经回路都有持久影响,以及对天然和药物奖赏消费的快感缺失样减少。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b67f/5991313/b6cf9fe768b1/gr1.jpg

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