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Midazolam, hippocampal function, and transitive inference: Reply to Greene

机译:咪达唑仑,海马功能和传递推论:回复Greene

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The transitive inference (TI) task assesses the ability to generalize learned knowledge to new contexts, and is thought to depend on the hippocampus (Dusek & Eichenbaum, 1997). Animals or humans learn in separate trials to choose stimulus A over B, B over C, C over D and D over E, via reinforcement feedback. Transitive responding based on the hierarchical structure A > B > C > D > E is then tested with the novel BD pair. We and others have argued that successful BD performance by animals – and even humans in some implicit studies – can be explained by simple reinforcement learning processes which do not depend critically on the hippocampus, but rather on the striatal dopamine system. We recently showed that the benzodiazepene midazolam, which is thought to disrupt hippocampal function, profoundly impaired human memory recall performance but actually enhanced implicit TI performance (Frank, O'Reilly & Curran, 2006). We posited that midazolam biased participants to recruit striatum during learning due to dysfunctional hippocampal processing, and that this change actually supported generalization of reinforcement values. Greene (2007) questions the validity of our pharmacological assumptions and argues that our conclusions are unfounded. Here we stand by our original hypothesis, which remains the most parsimonious account of the data, and is grounded by multiple lines of evidence.
机译:传递推理(TI)任务评估了将学习到的知识概括到新环境中的能力,并且被认为取决于海马(Dusek&Eichenbaum,1997)。动物或人类在单独的试验中学习通过增强反馈来选择刺激A而非B,B优于C,C优于D以及D优于E。然后,使用新的BD对测试基于层次结构A> B> C> D> E的传递响应。我们和其他人认为,动物的成功BD表现,甚至在一些隐性研究中甚至是人类,都可以通过简单的强化学习过程来解释,该过程并不严格依赖于海马体,而是依赖于纹状体多巴胺系统。我们最近发现,苯二氮卓咪达唑仑被认为会破坏海马功能,极大地削弱了人类记忆的回忆性能,但实际上却增强了隐式TI的性能(Frank,O'Reilly&Curran,2006)。我们认为,由于海马体功能障碍,咪达唑仑在学习过程中偏向参与者招募纹状体,而这一变化实际上支持了强化值的普遍化。 Greene(2007)质疑我们的药理假设的有效性,并认为我们的结论是没有根据的。在这里,我们支持我们的原始假设,该假设仍然是最简约的数据说明,并以多条证据为基础。

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