Couto-Pereira Natividade de Sá, Lampert Carine, Vieira Aline Dos Santos, Lazzaretti Camilla, Kincheski Grasielle Clotildes, Espejo Pablo Javier, Molina Victor Alejandro, Quillfeldt Jorge Alberto, Dalmaz Carla
Programa de Pós-graduação em Ciências Biológicas: Bioquímica, Instituto de Ciências Básicas da Saúde (ICBS), Universidade Federal do Rio Grande do Sul (UFRGS), Porto Alegre, Brazil.
Programa de Pós-graduação em Neurociências, Instituto de Ciências Básicas da Saúde (ICBS), Universidade Federal do Rio Grande do Sul (UFRGS), Porto Alegre, Brazil.
Front Mol Neurosci. 2019 May 28;12:134. doi: 10.3389/fnmol.2019.00134. eCollection 2019.
Early life experiences program lifelong responses to stress. In agreement, resilience and vulnerability to psychopathologies, such as posttraumatic stress disorder (PTSD), have been suggested to depend on the early background. New therapies have targeted memory reconsolidation as a strategy to modify the emotional valence of traumatic memories. Here, we used animal models to study the molecular mechanism through which early experiences may later affect aversive memory reconsolidation. Handling (H)-separation of pups from dams for 10 min-or maternal separation (MS) - 3-h separation-were performed from PDN1-10, using non-handled (NH) litters as controls. Adult males were trained in a contextual fear conditioning (CFC) task; 24 h later, a short reactivation session was conducted in the conditioned or in a novel context, followed by administration of midazolam 3 mg/kg i.p. (mdz), known to disturb reconsolidation, or vehicle; a test session was performed 24 h after. The immunocontent of relevant proteins was studied 15 and 60 min after memory reactivation in the dorsal hippocampus (dHc) and basolateral amygdala complex (BLA). Mdz-treated controls (NH) showed decreased freezing to the conditioned context, consistent with reconsolidation impairment, but H and MS were resistant to labilization. Additionally, MS males showed increased freezing to the novel context, suggesting fear generalization; H rats showed lower freezing than the other groups, in accordance with previous suggestions of reduced emotionality facing adversities. Increased levels of Zif268, GluN2B, β-actin and polyubiquitination found in the BLA of all groups suggest that memory reconsolidation was triggered. In the dHc, only NH showed increased Zif268 levels after memory retrieval; also, a delay in ERK1/2 activation was found in H and MS animals. We showed here that reconsolidation of a contextual fear memory is insensitive to interference by a GABAergic drug in adult male rats exposed to different neonatal experiences; surprisingly, we found no differences in the reconsolidation process in the BLA, but the dHc appears to suffer temporal desynchronization in the engagement of reconsolidation. Our results support a hippocampal-dependent mechanism for reconsolidation resistance in models of early experiences, which aligns with current hypotheses for the etiology of PTSD.
早期生活经历塑造了对压力的终身反应模式。与此观点一致的是,人们认为对诸如创伤后应激障碍(PTSD)等精神病理学的复原力和易感性取决于早期经历。新的治疗方法将记忆再巩固作为一种改变创伤性记忆情感效价的策略。在此,我们使用动物模型来研究早期经历可能在后期影响厌恶记忆再巩固的分子机制。从出生后第1天到第10天,对幼崽进行处理(H)——将幼崽与母鼠分离10分钟——或进行母鼠分离(MS)——分离3小时——以未处理(NH)的同窝幼崽作为对照。成年雄性大鼠接受情境恐惧条件反射(CFC)任务训练;24小时后,在条件化情境或新情境中进行短暂的再激活实验,随后腹腔注射3mg/kg咪达唑仑(mdz)(已知其会干扰再巩固)或注射溶剂;24小时后进行测试实验。在记忆再激活后15分钟和60分钟,研究背侧海马体(dHc)和基底外侧杏仁核复合体(BLA)中相关蛋白质的免疫含量。用mdz处理的对照组(NH)对条件化情境的僵立反应减少,这与再巩固受损一致,但H组和MS组对再激活具有抗性。此外,MS组雄性大鼠对新情境的僵立反应增加,表明出现了恐惧泛化;H组大鼠的僵立反应低于其他组,这与之前关于面对逆境时情绪性降低的观点一致。所有组的BLA中Zif268、GluN2B、β -肌动蛋白和多聚泛素化水平升高,表明记忆再巩固被触发。在dHc中,只有NH组在记忆提取后Zif268水平升高;此外,在H组和MS组动物中发现ERK1/2激活延迟。我们在此表明,在经历不同新生期经历的成年雄性大鼠中,情境恐惧记忆的再巩固对GABA能药物的干扰不敏感;令人惊讶的是,我们发现在BLA的再巩固过程中没有差异,但dHc在再巩固的参与中似乎存在时间不同步。我们的结果支持在早期经历模型中,海马体依赖的再巩固抗性机制,这与当前关于PTSD病因的假说一致。
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