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Evaluation of an angiotensin Type 1 receptor blocker on the reconsolidation of fear memory

机译:评估血管紧张素1型受体阻滞剂对恐惧记忆重新垄断的影响

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Inhibition of the angiotensin type 1 receptor (AT1R) has been shown to decrease fear responses in both humans and rodents. These effects are attributed to modulation of extinction learning, however the contribution of AT1R to alternative memory processes remains unclear. Using classic Pavlovian conditioning combined with radiotelemetry and whole-genome RNA sequencing, we evaluated the effects of the AT1R antagonist losartan on fear memory reconsolidation. Following the retrieval of conditioned auditory fear memory, animals were given a single intraperitoneal injection of losartan or saline. In response to the conditioned stimulus (CS), losartan-treated animals exhibited significantly less freezing at 24?h and 1 week; an effect that was dependent upon memory reactivation and independent of conditioned cardiovascular reactivity. Using an unbiased whole-genome RNA sequencing approach, transcriptomic analysis of the basolateral amygdala (BLA) identified losartan-dependent differences in gene expression during the reconsolidation phase. These findings demonstrate that post-retrieval losartan modifies behavioral and transcriptomic markers of conditioned fear memory, supporting an important regulatory role for this receptor in reconsolidation and as a potential pharmacotherapeutic target for maladaptive fear disorders such as PTSD.
机译:已经证明了血管紧张素1受体(AT1R)对人和啮齿动物的恐惧反应减少了血管紧张素型1受体(AT1R)。这些效果归因于消失学习的调制,但是AT1R对替代存储过程的贡献仍不清楚。使用经典的Pavlovian调理结合无线电记录和全基因组RNA测序,我们评估了AT1R拮抗剂氯沙坦对恐惧记忆重新溶解的影响。在检索条件听觉恐惧记忆之后,动物被腹膜内注射氯沙坦或盐水。响应于调节刺激(CS),氯沙坦处理的动物在24μm和1周时显着减少冻结;依赖于记忆重新激活和独立于调节心血管反应性的效果。使用无偏见的全基因组RNA测序方法,基底间杏仁菌(BLA)的转录组分析鉴定了重新溶解期期间基因表达的氯沙坦依赖性差异。这些研究结果表明,检索后氯沙坦改变了条件恐惧记忆的行为和转录组标志物,支持这种受体在重新染色中的重要调节作用以及作为PTSD的不良恐惧障碍的潜在药物治疗靶标。

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