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普萘洛尔对人类恐惧记忆表达的急性而非永久性影响。

Acute but Not Permanent Effects of Propranolol on Fear Memory Expression in Humans.

作者信息

Chalkia Anastasia, Weermeijer Jeroen, Van Oudenhove Lukas, Beckers Tom

机构信息

Centre for the Psychology of Learning and Experimental Psychopathology, Department of Psychology, KU Leuven, Leuven, Belgium.

Leuven Brain Institute, KU Leuven, Leuven, Belgium.

出版信息

Front Hum Neurosci. 2019 Feb 21;13:51. doi: 10.3389/fnhum.2019.00051. eCollection 2019.

Abstract

Experimental evidence in humans and non-human animals suggests that the administration of propranolol shortly after the retrieval of an emotional memory can lead to an attenuation of its later expression, a phenomenon known as post-reactivation amnesia. Using more potent amnestic drugs, post-reactivation amnesia has been shown in animals to be reversible by re-administration of the drug prior to memory retention testing. The latter finding suggests that, at least under some circumstances, post-reactivation amnesia may not reflect a disruption of reconsolidation (i.e., a memory storage deficit) but an acquired state-dependency of memory expression (i.e., a memory retrieval deficit that is relieved when the drug state is recreated during testing). We conducted a double-blind, placebo-controlled study to investigate whether the previously established amnestic effects of post-reactivation propranolol administration on memory retention in humans may similarly reflect a retrieval deficit. In four groups of participants, fear memories were first established through differential fear conditioning. One day later, a single presentation of the CS+ without shock was used to reactivate the memory in three of the four groups, followed by the administration of 40 mg Propranolol HCl (Groups PrPl and PrPr) or placebo (Group PlPl). Memory was not reactivated in the fourth group (Group NR). Another 24 h later, Propranolol HCl (Group PrPr) or placebo (Groups PrPl, PlPl, and NR) was again administered, followed by a test of memory retention (extinction testing) and recovery (reinstatement testing). We did not observe any effects of post-reactivation propranolol on memory retention; conditioned responding was similar for all groups at the start of retention testing and similarly sensitive to recovery through reinstatement. We did observe an acute effect of propranolol administration on fear-potentiated startle responding during retention testing in Group PrPr, where participants exhibited attenuated startle responses during extinction testing but similar sensitivity to reinstatement as participants in the other groups. While our findings fail to corroborate previous reports of propranolol-induced post-reactivation amnesia in humans, they do point to acute effects of propranolol administration on extinction performance.

摘要

人类和非人类动物的实验证据表明,在情感记忆恢复后不久给予普萘洛尔,可导致其后期表达减弱,这一现象被称为再激活后失忆。使用更强效的失忆药物,动物实验表明,在记忆保持测试前再次给药可使再激活后失忆可逆。后一项发现表明,至少在某些情况下,再激活后失忆可能并不反映重新巩固的破坏(即记忆存储缺陷),而是记忆表达的获得性状态依赖性(即当在测试期间重新创建药物状态时缓解的记忆检索缺陷)。我们进行了一项双盲、安慰剂对照研究,以调查再激活后给予普萘洛尔对人类记忆保持的先前确定的失忆效应是否同样反映检索缺陷。在四组参与者中,首先通过差异恐惧条件反射建立恐惧记忆。一天后,在四组中的三组中,仅呈现CS+而无电击来重新激活记忆,随后给予40毫克盐酸普萘洛尔(PrPl组和PrPr组)或安慰剂(PlPl组)。第四组(NR组)未重新激活记忆。再过24小时后,再次给予盐酸普萘洛尔(PrPr组)或安慰剂(PrPl组、PlPl组和NR组),随后进行记忆保持测试(消退测试)和恢复测试(恢复测试)。我们未观察到再激活后普萘洛尔对记忆保持有任何影响;在保持测试开始时,所有组的条件反应相似,并且对通过恢复进行的恢复同样敏感。我们确实观察到在PrPr组的保持测试期间,给予普萘洛尔对恐惧增强的惊吓反应有急性效应,该组参与者在消退测试期间表现出减弱的惊吓反应,但与其他组参与者对恢复的敏感性相似。虽然我们的研究结果未能证实先前关于普萘洛尔诱导人类再激活后失忆的报道,但它们确实指出了给予普萘洛尔对消退表现的急性效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e7b5/6394213/91f19cfebd58/fnhum-13-00051-g001.jpg

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