GABAergic circuit interaction between central amygdala and bed nucleus of the stria terminalis in lipopolysaccharide-induced despair-like behavior

IF 2.4 3区 医学 Q2 BEHAVIORAL SCIENCES Physiology & Behavior Pub Date : 2024-11-17 DOI:10.1016/j.physbeh.2024.114753
Yuka Tamura , Sakura Maeda , Haruna Takahashi , Yuta Aoto , Tohru Matsuki , Kenjiro Seki
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Abstract

Hyperexcitability of central amygdala (CeA) induces depressive symptoms. The bed nucleus of the stria terminalis (BNST) receives GABAergic input from the CeA. However, it remains unclear whether the GABAergic neurons in the CeA projecting to BNST contribute to major depression. Here, we investigated the roles of GABAergic neurons in CeA and BNST in lipopolysaccharide (LPS)-induced despair-like behavior. We generated adeno-associated virus vectors (AAV) carrying shRNA against Gad67 to knock down GAD67 expression in CeA (Gad67-KD-CeA) or BNST (Gad67-KD-BNST) in C57BL/6J male mice. Despair-like behavior was assessed by tail suspension test (TST) 24 h after LPS administration. Saline-treated Gad67-KD-CeA mice exhibited longer immobility during TST than saline-treated AAV-injected control (AAV-Cont) mice. Although LPS increased immobility time in AAV-Cont mice, it did not affect immobility time in Gad67-KD-CeA mice. While LPS did not affect the immobility time in Gad67-KD-BNST mice, it increased immobility time in AAV-Cont mice. We injected GFP-expressing AAV with a Dlx promoter, specifically expressed in GABAergic neurons, into CeA, and FluoroGold, a retrograde neuronal tracer, into the BNST. GFP signals associated with CeA GABAergic neurons were detected in the BNST, contacting c-fos and GAD67-expressed cells following LPS. We detected the FluoroGold signals in GAD67- and c-fos-expressed neurons in the CeA after LPS administration. Bilateral intra-BNST injection of muscimol (2 pmol), a GABAA receptor agonist, increased immobility time during TST. These findings suggest that LPS-decreased GABAergic activity in the CeA may lead to disinhibition of GABAergic interneurons in the BNST, resulting in GABAA receptor activation and subsequently induces despair-like behavior.
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中枢杏仁核与纹状体末端床核之间的GABA能回路在脂多糖诱发的绝望样行为中的相互作用
杏仁核中枢(CeA)的过度兴奋会诱发抑郁症状。纹状体末端床核(BNST)接受来自 CeA 的 GABA 能输入。然而,CeA中投射到BNST的GABA能神经元是否会导致重度抑郁症,目前仍不清楚。在这里,我们研究了CeA和BNST中的GABA能神经元在脂多糖(LPS)诱导的绝望样行为中的作用。我们生成了携带针对 Gad67 的 shRNA 的腺相关病毒载体(AAV),以敲除 C57BL/6J 雄性小鼠 CeA(Gad67-KD-CeA)或 BNST(Gad67-KD-BNST)中 GAD67 的表达。在给予 LPS 24 小时后,通过尾悬试验(TST)评估绝望样行为。盐水处理的Gad67-KD-CeA小鼠与盐水处理的AAV注射对照组(AAV-Cont)小鼠相比,在TST期间表现出更长的静止不动时间。虽然 LPS 延长了 AAV-Cont 小鼠的固定时间,但并不影响 Gad67-KD-CeA 小鼠的固定时间。虽然 LPS 不影响 Gad67-KD-BNST 小鼠的移动时间,但却增加了 AAV-Cont 小鼠的移动时间。我们将带有 Dlx 启动子的表达 GFP 的 AAV(专门在 GABA 能神经元中表达)注入 CeA,并将逆行神经元示踪剂 FluoroGold 注入 BNST。在 BNST 中检测到了与 CeA GABA 能神经元相关的 GFP 信号,这些信号在 LPS 后与 c-fos 和 GAD67 表达的细胞接触。注射 LPS 后,我们在 CeA 的 GAD67 和 c-fos 表达神经元中检测到了荧光金信号。在双侧脑皮质内注射麝香草酚(2 pmol)(一种 GABAA 受体激动剂)可增加 TST 期间的静止时间。这些研究结果表明,LPS降低了CeA中的GABA能活性,可能会导致BNST中的GABA能中间神经元失去抑制,从而导致GABAA受体激活,进而诱发绝望样行为。
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来源期刊
Physiology & Behavior
Physiology & Behavior 医学-行为科学
CiteScore
5.70
自引率
3.40%
发文量
274
审稿时长
47 days
期刊介绍: Physiology & Behavior is aimed at the causal physiological mechanisms of behavior and its modulation by environmental factors. The journal invites original reports in the broad area of behavioral and cognitive neuroscience, in which at least one variable is physiological and the primary emphasis and theoretical context are behavioral. The range of subjects includes behavioral neuroendocrinology, psychoneuroimmunology, learning and memory, ingestion, social behavior, and studies related to the mechanisms of psychopathology. Contemporary reviews and theoretical articles are welcomed and the Editors invite such proposals from interested authors.
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