Huerta Sanchez Laura L, Sankaran Mathangi, Li Taylor L, Doan Hoa, Chiu Alvin, Shulman Eleanora, Shab Gabriella, Kippin Tod E, Szumlinski Karen K
Department of Psychological and Brain Sciences, University of California, Santa Barbara, Santa Barbara, CA, United States.
Department of Molecular, Cellular and Developmental Biology, University of California, Santa Barbara, Santa Barbara, CA, United States.
Front Psychiatry. 2023 Jan 4;13:1031585. doi: 10.3389/fpsyt.2022.1031585. eCollection 2022.
Incubation of drug-craving refers to a time-dependent increase in drug cue-elicited craving that occurs during protracted withdrawal. Historically, rat models of incubated cocaine craving employed extended-access (typically 6 h/day) intravenous drug self-administration (IV-SA) procedures, although incubated cocaine craving is reported to occur following shorter-access IV-SA paradigms. The notoriously low-throughput of extended-access IV-SA prompted us to determine whether two different short-access IV-SA procedures akin to those in the literature result in qualitatively similar changes in glutamate receptor expression and the activation of downstream signaling molecules within prefrontal cortex (PFC) subregions as those reported previously by our group under 6h-access conditions.
For this, adult, male Sprague-Dawley rats were trained to intravenously self-administer cocaine for 2 h/day for 10 consecutive days (2-h model) or for 6 h on day 1 and 2 h/day for the remaining 9 days of training (Mixed model). A sham control group was also included that did not self-administer cocaine.
On withdrawal day 3 or 30, rats were subjected to a 2-h test of cue-reinforced responding in the absence of cocaine and a time-dependent increase in drug-seeking was observed under both IV-SA procedures. Immunoblotting of brain tissue collected immediately following the cue test session indicated elevated phospho-Akt1, phospho-CaMKII and Homer2a/b expression within the prelimbic subregion of the PFC of cocaine-incubated rats. However, we failed to detect incubation-related changes in Group 1 metabotropic glutamate receptor or ionotropic glutamate receptor subunit expression in either subregion.
These results highlight further a role for Akt1-related signaling within the prelimbic cortex in driving incubated cocaine craving, and provide novel evidence supporting a potential role also for CaMKII-dependent signaling through glutamate receptors in this behavioral phenomenon.
药物渴求潜伏期是指在长期戒断期间,药物线索引发的渴求随时间增加的现象。从历史上看,可卡因渴求潜伏期的大鼠模型采用延长给药时间(通常每天6小时)的静脉内药物自我给药(IV-SA)程序,不过据报道,在较短给药时间的IV-SA范式后也会出现可卡因渴求潜伏期。延长给药时间的IV-SA通量极低,促使我们确定两种类似于文献中的不同短给药时间IV-SA程序,是否会导致前额叶皮质(PFC)亚区域内谷氨酸受体表达以及下游信号分子激活发生定性相似的变化,如同我们小组之前报道的在6小时给药条件下所发生的变化一样。
为此,成年雄性Sprague-Dawley大鼠接受训练,连续10天每天静脉内自我给药可卡因2小时(2小时模型),或在第1天给药6小时,其余9天训练每天给药2小时(混合模型)。还包括一个未自我给药可卡因的假对照组。
在戒断第3天或第30天,大鼠在无可卡因的情况下接受2小时线索强化反应测试,在两种IV-SA程序下均观察到药物寻求行为随时间增加。线索测试结束后立即收集的脑组织免疫印迹显示,可卡因潜伏期大鼠PFC前边缘亚区域内磷酸化Akt1、磷酸化CaMKII和Homer2a/b表达升高。然而,我们未能在任一亚区域检测到第1组代谢型谷氨酸受体或离子型谷氨酸受体亚基表达与潜伏期相关的变化。
这些结果进一步突出了前边缘皮质内Akt1相关信号在驱动可卡因渴求潜伏期方面的作用,并提供了新的证据,支持CaMKII依赖的信号通过谷氨酸受体在这一行为现象中也具有潜在作用。
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