Garcia-Keller C, Kupchik Y M, Gipson C D, Brown R M, Spencer S, Bollati F, Esparza M A, Roberts-Wolfe D J, Heinsbroek J A, Bobadilla A-C, Cancela L M, Kalivas P W
Department of Neuroscience, Medical University of South Carolina, Charleston, SC, USA.
IFEC-CONICET, Departamento de Farmacología, Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, Córdoba, Argentina.
Mol Psychiatry. 2016 Aug;21(8):1063-9. doi: 10.1038/mp.2015.151. Epub 2015 Oct 6.
There is substantial comorbidity between stress disorders and substance use disorders (SUDs), and acute stress augments the locomotor stimulant effect of cocaine in animal models. Here we endeavor to understand the neural underpinnings of comorbid stress disorders and drug use by determining whether the glutamatergic neuroadaptations that characterize cocaine self-administration are induced by acute stress. Rats were exposed to acute (2 h) immobilization stress, and 3 weeks later the nucleus accumbens core was examined for changes in glutamate transport, glutamate-mediated synaptic currents and dendritic spine morphology. We also determined whether acute stress potentiated the acquisition of cocaine self-administration. Acute stress produced an enduring reduction in glutamate transport and potentiated excitatory synapses on medium spiny neurons. Acute stress also augmented the acquisition of cocaine self-administration. Importantly, by restoring glutamate transport in the accumbens core with ceftriaxone the capacity of acute stress to augment the acquisition of cocaine self-administration was abolished. Similarly, ceftriaxone treatment prevented stress-induced potentiation of cocaine-induced locomotor activity. However, ceftriaxone did not reverse stress-induced synaptic potentiation, indicating that this effect of stress exposure did not underpin the increased acquisition of cocaine self-administration. Reversing acute stress-induced vulnerability to self-administer cocaine by normalizing glutamate transport poses a novel treatment possibility for reducing comorbid SUDs in stress disorders.
应激障碍与物质使用障碍(SUDs)之间存在大量共病现象,并且在动物模型中,急性应激会增强可卡因的运动兴奋作用。在此,我们试图通过确定可卡因自我给药所特有的谷氨酸能神经适应性是否由急性应激诱导,来理解共病应激障碍和药物使用的神经基础。将大鼠暴露于急性(2小时)固定应激,3周后检查伏隔核核心区谷氨酸转运、谷氨酸介导的突触电流和树突棘形态的变化。我们还确定了急性应激是否增强了可卡因自我给药的习得。急性应激导致谷氨酸转运持续减少,并增强了中等棘状神经元上的兴奋性突触。急性应激还增强了可卡因自我给药的习得。重要的是,通过用头孢曲松恢复伏隔核核心区的谷氨酸转运,急性应激增强可卡因自我给药习得的能力被消除。同样,头孢曲松治疗可防止应激诱导的可卡因诱导的运动活动增强。然而,头孢曲松并未逆转应激诱导的突触增强,这表明应激暴露的这种效应并非可卡因自我给药习得增加的基础。通过使谷氨酸转运正常化来逆转急性应激诱导的自我给药可卡因的易感性,为减少应激障碍中共病的SUDs提供了一种新的治疗可能性。
