Feil Family Brain and Mind Research Institute, Weill Cornell Medicine, New York, NY, 10065, USA.
Linda and Jack Gill Center for Biomolecular Science, Dept. of Psychological and Brain Sciences, Indiana University, Bloomington, IN, 47404, USA.
Neuropsychopharmacology. 2020 Jan;45(2):374-383. doi: 10.1038/s41386-019-0466-9. Epub 2019 Jul 19.
Adolescence is a vulnerable period of development when limbic connection of the prefrontal cortex (PFC) involved in emotional processing may be rendered dysfunctional by chronic exposure to delta-9-tetrahydrocannabinol (∆9-THC), the major psychoactive compound in marijuana. Cannabinoid-1 receptors (CB1Rs) largely mediate the central neural effects of ∆9-THC and endocannabinoids that regulate NMDA receptor-dependent synaptic plasticity of glutamatergic synapses in the prelimbic prefrontal cortex (PL-PFC). Thus, chronic occupancy of CB1Rs by ∆9-THC during adolescence may competitively decrease the functional expression and activity of NMDA receptors in the mature PL-PFC. We used a multidisciplinary approach to test this hypothesis in adult C57BL/6J male mice that received vehicle or ∆9-THC in escalating doses (2.5-10 mg/kg/ip) through adolescence (postnatal day 29-43). In comparison with vehicle, the mice receiving ∆9-THC showed a hyperpolarized resting membrane potential, decreased spontaneous firing rate, increased current-induced firing threshold, and decreased depolarizing response to NMDA in deep-layer PL-PFC neurons analyzed by current-clamp recordings. Electron microscopic immunolabeling in the PL-PFC of adult mice that had received Δ9-THC only during adolescence showed a significant (1) decrease in the extrasynaptic plasmalemmal density of obligatory GluN1-NMDA subunits in dendrites of all sizes and (2) a shift from cytoplasmic to plasmalemmal distribution of GluN1 in large dendrites receiving mainly inhibitory-type synapses from CB1R-labeled terminals. From these results and concomitant behavioral studies, we conclude that social dysfunctions resulting from excessive intake of ∆9-THC in the increasingly available marijuana products used by male teens may largely reflect circuit defects in PL-PFC networks communicating through endocannabinoid-regulated NMDA receptors.
青春期是一个发育脆弱的时期,此时前额叶皮质(PFC)的边缘连接可能由于慢性接触大麻中主要的精神活性化合物Δ9-四氢大麻酚(∆9-THC)而变得功能失调。大麻素 1 型受体(CB1Rs)在很大程度上介导∆9-THC 和内源性大麻素对前额叶皮质前扣带回(PL-PFC)中谷氨酸能突触 NMDA 受体依赖性突触可塑性的中枢神经作用。因此,青春期期间∆9-THC 对 CB1Rs 的慢性占据可能会竞争性地降低成熟 PL-PFC 中 NMDA 受体的功能表达和活性。我们使用多学科方法在成年 C57BL/6J 雄性小鼠中测试了这一假说,这些小鼠在青春期(出生后第 29-43 天)接受了递增剂量的载体或∆9-THC(2.5-10mg/kg/ip)。与载体相比,接受∆9-THC 的小鼠在电流钳记录分析的 PL-PFC 深层神经元中表现出超极化的静息膜电位、自发放电率降低、电流诱导的放电阈值增加以及对 NMDA 的去极化反应减少。在仅在青春期接受 Δ9-THC 的成年小鼠的 PL-PFC 中进行的电子显微镜免疫标记显示,(1)所有大小的树突中必需的 GluN1-NMDA 亚基的突触外质膜密度显著降低,(2)从细胞质到 GluN1 的质膜分布的转变在接收主要来自 CB1R 标记末端的抑制型突触的大树突中。从这些结果和伴随的行为研究中,我们得出结论,由于男性青少年越来越多地使用大麻制品中过量摄入∆9-THC 而导致的社交功能障碍,在很大程度上反映了通过内源性大麻素调节的 NMDA 受体进行通讯的 PL-PFC 网络中的电路缺陷。
