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慢性间歇性乙醇摄入及戒断会抑制向基底外侧杏仁核主神经元不同群体释放的诱发型和自发性γ-氨基丁酸。

Chronic Intermittent Ethanol and Withdrawal Suppress Evoked and Spontaneous GABA Release Onto Distinct Populations of Basolateral Amygdala Principal Neurons.

作者信息

Price Michaela E, Egido-Betancourt Hailey X, Sizer Sarah E, Parrish Brian P, Alexander Nancy J, Raab-Graham Kimberly F, McCool Brian A

机构信息

Department of Translational Neuroscience, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.

出版信息

Addict Biol. 2025 Sep;30(9):e70080. doi: 10.1111/adb.70080.

DOI:10.1111/adb.70080
PMID:40977005
Abstract

Unique populations of basolateral amygdala (BLA) neurons regulate anxiety and reward through projections targeting downstream regions like the bed nucleus of the stria terminalis (BNST) and nucleus accumbens (NAC). We showed previously that withdrawal from chronic ethanol exposure (CIE/WD) produced population- and sex-specific alterations to distinct glutamatergic inputs. The current study examined GABAergic function in these distinct populations (BLA and BLA neurons). We found that CIE/WD diminished feed-forward GABA release from lateral paracapsular cells (LPCs) specifically onto male BLA neurons. Pharmacological manipulations showed this dysregulation was caused by the enhanced activity of μ-opioid receptors. CIE/WD did not alter evoked GABA release from local interneurons onto either population. However, females expressed greater GABA release from these local interneurons compared to males. Immunostaining and confocal microscopy revealed lower colocalization between the GABA vesicular transporter, vGAT and parvalbumin in females, indicating that greater GABA releases from local interneurons in this sex may be a compensatory response to lower levels of perisomatic innervation by PV interneurons. Consistent with this, there were no sex differences related to spontaneous GABAergic synaptic events although CIE/WD decreased their frequency specifically in BLA neurons from both sexes. Altogether, these findings demonstrate that CIE/WD dynamically alters GABAergic function in an input-, sex- and population-specific fashion. Moreover, there are basal sex differences in both the anatomy of BLA GABAergic synapses and their function.

摘要

基底外侧杏仁核(BLA)神经元的独特群体通过靶向终纹床核(BNST)和伏隔核(NAC)等下游区域的投射来调节焦虑和奖赏。我们之前表明,慢性乙醇暴露戒断(CIE/WD)会对不同的谷氨酸能输入产生群体和性别特异性改变。当前研究检查了这些不同群体(BLA和BLA神经元)中的GABA能功能。我们发现CIE/WD特异性地减少了外侧囊周细胞(LPCs)向雄性BLA神经元的前馈GABA释放。药理学操作表明这种失调是由μ-阿片受体活性增强引起的。CIE/WD并未改变局部中间神经元向这两个群体诱发的GABA释放。然而,与雄性相比,雌性从这些局部中间神经元释放出更多的GABA。免疫染色和共聚焦显微镜显示,雌性中GABA囊泡转运体vGAT与小白蛋白的共定位较低,表明该性别中局部中间神经元释放更多的GABA可能是对小白蛋白中间神经元躯体周围神经支配水平较低的一种代偿反应。与此一致,尽管CIE/WD特异性降低了两性BLA神经元中自发GABA能突触事件的频率,但在自发GABA能突触事件方面没有性别差异。总之,这些发现表明CIE/WD以输入、性别和群体特异性方式动态改变GABA能功能。此外,BLA GABA能突触的解剖结构及其功能在基础水平上存在性别差异。

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