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社交隔离期间皮质边缘区别孕烯醇酮表达降低会增强情境性恐惧:一种与创伤后应激障碍相关的模型。

Decreased corticolimbic allopregnanolone expression during social isolation enhances contextual fear: A model relevant for posttraumatic stress disorder.

作者信息

Pibiri Fabio, Nelson Marianela, Guidotti Alessandro, Costa Erminio, Pinna Graziano

机构信息

Psychiatric Institute, Department of Psychiatry, University of Illinois, 1601 West Taylor Street, Chicago, IL 60612, USA.

出版信息

Proc Natl Acad Sci U S A. 2008 Apr 8;105(14):5567-72. doi: 10.1073/pnas.0801853105. Epub 2008 Apr 7.

Abstract

Mice subjected to social isolation (3-4 weeks) exhibit enhanced contextual fear responses and impaired fear extinction. These responses are time-related to a decrease of 5alpha-reductase type I (5alpha-RI) mRNA expression and allopregnanolone (Allo) levels in selected neurons of the medial prefrontal cortex, hippocampus, and basolateral amygdala. Of note, the cued fear response was not different between group housed and socially isolated mice. In socially isolated mice, S-norfluoxetine, a selective brain steroidogenic stimulant (SBSS), in doses (0.45-1.8 mumol/kg) that increase brain Allo levels but fail to inhibit serotonin reuptake, greatly attenuates enhanced contextual fear response. SKF 105,111 (a potent 5alpha-RI inhibitor) decreases corticolimbic Allo levels and enhances the contextual fear response in group housed mice, which suggests that social isolation alters emotional responses by reducing the positive allosteric modulation of Allo at GABA(A) receptors in corticolimbic circuits. Thus, these procedures model emotional hyperreactivity, including enhanced contextual fear and impaired contextual fear extinction, which also is observed in posttraumatic stress disorder (PTSD) patients. A recent clinical study reported that cerebrospinal fluid Allo levels also are down-regulated in PTSD patients and correlate negatively with PTSD symptoms and negative mood. Thus, protracted social isolation of mice combined with tests of fear conditioning may be a suitable model to study emotional behavioral components associated with neurochemical alterations relating to PTSD. Importantly, drugs like SBSSs, which rapidly increase corticolimbic Allo levels, normalize the exaggerated contextual fear responses resulting from social isolation, suggesting that selective activation of neurosteroidogenesis may be useful in PTSD therapy.

摘要

遭受社会隔离(3 - 4周)的小鼠表现出增强的情境恐惧反应和恐惧消退受损。这些反应与内侧前额叶皮质、海马体和基底外侧杏仁核中特定神经元的I型5α - 还原酶(5α - RI)mRNA表达及别孕烷醇酮(Allo)水平降低在时间上相关。值得注意的是,群居小鼠和社会隔离小鼠之间的线索性恐惧反应没有差异。在社会隔离的小鼠中,S - 去甲氟西汀,一种选择性脑类固醇生成刺激剂(SBSS),以能增加脑内Allo水平但不能抑制5 - 羟色胺再摄取的剂量(0.45 - 1.8 μmol/kg),可大大减弱增强的情境恐惧反应。SKF 105,111(一种有效的5α - RI抑制剂)降低皮质边缘系统的Allo水平,并增强群居小鼠的情境恐惧反应,这表明社会隔离通过减少皮质边缘回路中Allo对GABA(A)受体的正构变构调节来改变情绪反应。因此,这些程序模拟了情绪反应过度,包括增强的情境恐惧和情境恐惧消退受损,这在创伤后应激障碍(PTSD)患者中也有观察到。最近一项临床研究报告称,PTSD患者脑脊液中的Allo水平也下调,且与PTSD症状和负性情绪呈负相关。因此,小鼠的长期社会隔离结合恐惧条件测试可能是研究与PTSD相关神经化学改变的情绪行为成分的合适模型。重要的是,像SBSS这样能迅速增加皮质边缘系统Allo水平的药物,可使因社会隔离导致的过度情境恐惧反应正常化,这表明神经类固醇生成的选择性激活可能对PTSD治疗有用。

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