Wheelan Nicola, Seckl Jonathan R, Yau Joyce L W
Centre for Cardiovascular Science, University of Edinburgh, United Kingdom.
Centre for Cardiovascular Science, University of Edinburgh, United Kingdom; Centre for Clinical Brain Sciences, University of Edinburgh, United Kingdom.
Psychoneuroendocrinology. 2022 Dec;146:105945. doi: 10.1016/j.psyneuen.2022.105945. Epub 2022 Sep 27.
Post-traumatic stress disorder (PTSD) is characterized by the co-existence of a persistent strong memory of the traumatic experience and amnesia for the peritraumatic context. Most animal models, however, fail to account for the contextual amnesia which is considered to play a critical role in the etiology of PTSD intrusive memories. It is also unclear how aging affects PTSD-like memory. Glucocorticoids alter the formation and retention of fear-associated memory. Here, we investigated whether a deficiency of 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) (an intracellular glucocorticoid generating enzyme) and aging modulates fear conditioning and PTSD-like memory in mice. We first measured memory in 6 months and 24 months old 11β-HSD1 deficient (HSD1 KO) and wildtype (WT) mice following paired tone-shock fear conditioning. Then, separate groups of mice were exposed to restraint stress immediately after unpaired tone-shock contextual fear conditioning. Compared with young controls, aged WT mice exhibited enhanced auditory cued fear memory, but contextual fear memory was not different. Contextual fear memory retention was attenuated in both young and aged HSD1 KO mice. In contrast, auditory cued fear memory was reduced 24 h after training only in aged HSD1 KO mice. When fear conditioned with stress, WT mice displayed PTSD-like memory (i.e., increased fear to tone not predictive of shock and reduced fear to 'aversive' conditioning context); this was unchanged with aging. In contrast, young HSD1 KO mice fear conditioned with stress showed normal fear memory (i.e., increased fear response to conditioning context), as observed in WT mice fear conditioned alone. While aged HSD1 KO mice fear conditioned with stress also displayed normal contextual fear memory, the fear response to the 'safe' tone remained. Thus, a deficiency of 11β-HSD1 protects against both amnesia for the conditioning context and hypermnesia for a salient tone in young adult mice but only contextual amnesia is prevented in aged mice. These results suggest that brain 11β-HSD1 generated glucocorticoids make a significant contribution to fear conditioning and PTSD-like memory. 11β-HSD1 inhibition may be useful in prevention and/or treatment of PTSD.
创伤后应激障碍(PTSD)的特征是创伤经历的强烈记忆持续存在,同时对创伤周围环境失忆。然而,大多数动物模型未能考虑到情境性失忆,而情境性失忆被认为在PTSD侵入性记忆的病因学中起关键作用。衰老如何影响类似PTSD的记忆也尚不清楚。糖皮质激素会改变与恐惧相关记忆的形成和保留。在此,我们研究了11β-羟基类固醇脱氢酶1型(11β-HSD1,一种细胞内糖皮质激素生成酶)的缺乏和衰老是否会调节小鼠的恐惧条件反射和类似PTSD的记忆。我们首先在6个月和24个月大的11β-HSD1缺陷型(HSD1 KO)和野生型(WT)小鼠中进行配对音-休克恐惧条件反射后测量记忆。然后,在未配对音-休克情境恐惧条件反射后,将单独的小鼠组立即暴露于束缚应激。与年轻对照组相比,老年WT小鼠表现出增强的听觉线索恐惧记忆,但情境恐惧记忆没有差异。年轻和老年HSD1 KO小鼠的情境恐惧记忆保持均减弱。相比之下,仅在老年HSD1 KO小鼠中,训练后24小时听觉线索恐惧记忆减少。当用应激进行恐惧条件反射时,WT小鼠表现出类似PTSD的记忆(即对不预示休克的音调恐惧增加,对“厌恶”条件反射情境的恐惧减少);这不会随衰老而改变。相比之下,如在单独进行恐惧条件反射的WT小鼠中观察到的那样,用应激进行恐惧条件反射的年轻HSD1 KO小鼠表现出正常的恐惧记忆(即对条件反射情境的恐惧反应增加)。虽然用应激进行恐惧条件反射的老年HSD1 KO小鼠也表现出正常的情境恐惧记忆,但对“安全”音调的恐惧反应仍然存在。因此,11β-HSD1的缺乏可防止年轻成年小鼠对条件反射情境的失忆和对显著音调的记忆增强,但在老年小鼠中仅能防止情境性失忆。这些结果表明,大脑中由11β-HSD1生成的糖皮质激素对恐惧条件反射和类似PTSD的记忆有重大贡献。抑制11β-HSD1可能有助于预防和/或治疗PTSD。
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