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多发性硬化症损伤会影响记忆,这些损伤与一个连接的记忆回路有关。

Multiple sclerosis lesions that impair memory map to a connected memory circuit.

机构信息

Division of Cognitive and Behavioral Neurology, Brigham and Women's Hospital, 60 Fenwood Road, 9016H, Boston, MA, 02115, USA.

Department of Neurology, Brigham and Women's Hospital, Boston, USA.

出版信息

J Neurol. 2023 Nov;270(11):5211-5222. doi: 10.1007/s00415-023-11907-8. Epub 2023 Aug 2.

Abstract

BACKGROUND

Nearly 1 million Americans are living with multiple sclerosis (MS) and 30-50% will experience memory dysfunction. It remains unclear whether this memory dysfunction is due to overall white matter lesion burden or damage to specific neuroanatomical structures. Here we test if MS memory dysfunction is associated with white matter lesions to a specific brain circuit.

METHODS

We performed a cross-sectional analysis of standard structural images and verbal memory scores as assessed by immediate recall trials from 431 patients with MS (mean age 49.2 years, 71.9% female) enrolled at a large, academic referral center. White matter lesion locations from each patient were mapped using a validated algorithm. First, we tested for associations between memory dysfunction and total MS lesion volume. Second, we tested for associations between memory dysfunction and lesion intersection with an a priori memory circuit derived from stroke lesions. Third, we performed mediation analyses to determine which variable was most associated with memory dysfunction. Finally, we performed a data-driven analysis to derive de-novo brain circuits for MS memory dysfunction using both functional (n = 1000) and structural (n = 178) connectomes.

RESULTS

Both total lesion volume (r = 0.31, p < 0.001) and lesion damage to our a priori memory circuit (r = 0.34, p < 0.001) were associated with memory dysfunction. However, lesion damage to the memory circuit fully mediated the association of lesion volume with memory performance. Our data-driven analysis identified multiple connections associated with memory dysfunction, including peaks in the hippocampus (T = 6.05, family-wise error p = 0.000008), parahippocampus, fornix and cingulate. Finally, the overall topography of our data-driven MS memory circuit matched our a priori stroke-derived memory circuit.

CONCLUSIONS

Lesion locations associated with memory dysfunction in MS map onto a specific brain circuit centered on the hippocampus. Lesion damage to this circuit fully mediated associations between lesion volume and memory. A circuit-based approach to mapping MS symptoms based on lesions visible on standard structural imaging may prove useful for localization and prognosis of higher order deficits in MS.

摘要

背景

近 100 万美国人患有多发性硬化症(MS),其中 30-50%会出现记忆功能障碍。目前尚不清楚这种记忆功能障碍是由于总体白质病变负担还是特定神经解剖结构的损伤引起的。在这里,我们测试 MS 记忆功能障碍是否与特定大脑回路的白质病变有关。

方法

我们对 431 名在大型学术转诊中心就诊的 MS 患者(平均年龄 49.2 岁,71.9%为女性)的标准结构图像和即时回忆试验评估的言语记忆评分进行了横断面分析。使用验证算法对每位患者的白质病变位置进行了映射。首先,我们测试了记忆功能障碍与 MS 病变总容积之间的相关性。其次,我们测试了记忆功能障碍与从卒中病变衍生的前序记忆回路的病变交叉之间的相关性。第三,我们进行了中介分析,以确定与记忆功能障碍最相关的变量。最后,我们进行了一项数据驱动分析,使用功能(n=1000)和结构(n=178)连接组学为 MS 记忆障碍导出全新的大脑回路。

结果

总病变体积(r=0.31,p<0.001)和我们前序记忆回路的病变损伤(r=0.34,p<0.001)与记忆功能障碍均相关。然而,病变对记忆回路的损伤完全介导了病变体积与记忆表现之间的关联。我们的数据驱动分析确定了与记忆功能障碍相关的多个连接,包括海马体(T=6.05,全脑错误率 p=0.000008)、海马旁回、穹窿和扣带回的峰值。最后,我们数据驱动的 MS 记忆回路的整体拓扑结构与我们从卒中衍生的前序记忆回路相匹配。

结论

与 MS 记忆功能障碍相关的病变位置映射到以海马体为中心的特定大脑回路。该回路的病变损伤完全介导了病变体积与记忆之间的关联。基于标准结构成像上可见的病变对 MS 症状进行基于回路的映射可能有助于定位和预测 MS 中更高阶缺陷。

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