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Oxytocin signaling in basolateral and central amygdala nuclei differentially regulates the acquisition expression and extinction of context-conditioned fear in rats

机译:大鼠基底外侧和中央杏仁核中的催产素信号差异调节大鼠条件性恐惧的获取表达和消退

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摘要

The present study investigated how oxytocin (OT) signaling in the central (CeA) and basolateral (BLA) amygdala affects acquisition, expression, and extinction of context-conditioned fear (freezing) in rats. In the first set of experiments, acquisition of fear to a shocked context was impaired by a preconditioning infusion of synthetic OT into the CeA (Experiment 1) or BLA (Experiment 2). In the second set of experiments, expression of context fear was enhanced by a pre- or post-extinction CeA infusion of synthetic OT (Experiments 3–6) or a selective OT receptor agonist, TGOT (Experiment 4). This enhancement of fear was blocked by coadministration of an OT receptor antagonist, OTA (Experiment 5) and context fear was suppressed by administration of the antagonist alone (Experiment 6). In the third set of experiments, expression of context fear was suppressed, not enhanced, by a preextinction BLA infusion of synthetic OT or a selective OT receptor agonist, TGOT (Experiments 7 and 8). This suppression of fear was blocked by coadministration of the OT receptor antagonist, OTA (Experiment 8). Taken together, these findings show that the involvement of the CeA and BLA in expression and extinction of context-conditioned fear is dissociable, and imply a critical role for oxytocin signaling in amygdala-based regulation of aversive learning.
机译:本研究调查了中枢(CeA)和基底外侧(BLA)杏仁核中的催产素(OT)信号如何影响大鼠的情境条件恐惧(冻结)的获取,表达和消灭。在第一组实验中,通过将预先合成的OT预先注入CeA(实验1)或BLA(实验2)中,损害了对震惊环境的恐惧感。在第二组实验中,通过灭绝前或灭绝后的CeA注入合成OT(实验3-6)或选择性OT受体激动剂TGOT(实验4),可以增强语境恐惧的表达。 OT受体拮抗剂OTA的共同给药可阻止这种恐惧感的增强(实验5),而单独给予拮抗剂可抑制背景恐惧感(实验6)。在第三组实验中,通过绝灭前BLA输注合成OT或选择性OT受体激动剂TGOT来抑制而不是增强背景恐惧的表达(实验7和8)。 OT受体拮抗剂OTA的并用阻止了对恐惧的抑制(实验8)。综上所述,这些发现表明,CeA和BLA参与表达和消灭情境条件的恐惧是不可分割的,并暗示催产素信号在基于杏仁核的厌恶性学习调节中的关键作用。

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