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人类短暂性海马 CA1 损伤会损害模式分离能力。

Transient hippocampal CA1 lesions in humans impair pattern separation performance.

机构信息

Memory Disorders and Plasticity Group, Department of Neurology, University Hospital Schleswig-Holstein, Kiel, University of Kiel, Kiel, Germany.

Department of Psychology, Clinical Psychology and Psychotherapy, University of Kiel, Kiel, Germany.

出版信息

Hippocampus. 2019 Aug;29(8):736-747. doi: 10.1002/hipo.23073. Epub 2019 Jan 31.

Abstract

Day-to-day life involves the perception of events that resemble one another. For the sufficient encoding and retrieval of similar information, the hippocampus provides two essential computational processes. Pattern separation refers to the differentiation of overlapping memory representations, whereas pattern completion reactivates memories based on noisy or degraded input. Evidence from human and rodent studies suggest that pattern separation specifically relies on neuronal ensemble activity in hippocampal subnetworks in the dentate gyrus and CA3. Although a role for CA1 in pattern separation has been shown in animal models, its contribution in the human hippocampus remains elusive. In order to elucidate the contribution of CA1 neurons to pattern separation, we examined 14 patients with an acute transient global amnesia (TGA), a rare self-limiting dysfunction of the hippocampal system showing specific lesions to CA1. Patients' pattern separation performance was tested during the acute amnestic phase and follow-up using an established mnemonic similarity test. Patients in the acute phase showed a profound deficit in pattern separation (p < .05) as well as recognition memory (p < .001) that recovered during follow-up. Specifically, patients tested in a later stage of the amnesia were less impaired in pattern separation than in recognition memory. Considering the time dependency of lesion-associated hippocampal deficits in early and late acute stages of the TGA, we showed that the pattern separation function recovered significantly earlier than recognition memory. Our results provide causal evidence that hippocampal CA1 neurons are critical to pattern separation performance in humans.

摘要

日常生活涉及到对相似事件的感知。为了充分编码和检索相似信息,海马体提供了两个重要的计算过程。模式分离是指对重叠记忆表征的区分,而模式完成则根据噪声或退化的输入重新激活记忆。来自人类和啮齿动物研究的证据表明,模式分离特别依赖于海马体齿状回和 CA3 中海马体亚网络中的神经元集合活动。尽管动物模型已经表明 CA1 在模式分离中具有作用,但它在人类海马体中的贡献仍然难以捉摸。为了阐明 CA1 神经元对模式分离的贡献,我们检查了 14 名患有急性短暂性全面遗忘症(TGA)的患者,这是一种罕见的、自限性的海马体系统功能障碍,表现为 CA1 的特定损伤。使用已建立的记忆相似性测试,在急性遗忘阶段和随访期间测试患者的模式分离表现。在急性阶段的患者表现出明显的模式分离缺陷(p<0.05)以及识别记忆缺陷(p<0.001),这些缺陷在随访期间得到了恢复。具体来说,在遗忘症的后期阶段接受测试的患者在模式分离方面的损伤程度低于识别记忆。考虑到 TGA 早期和晚期急性阶段与损伤相关的海马体缺陷的时间依赖性,我们表明模式分离功能的恢复明显早于识别记忆。我们的结果提供了因果证据,表明海马体 CA1 神经元对人类的模式分离表现至关重要。

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