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临床高危精神病患者的失匹配负波:无渐进性衰退证据

Mismatch Negativity in Subjects at Clinical High Risk for Psychosis: No Evidence of Progressive Decline.

作者信息

Jang Jiseon, Choe Eugenie, Ha Minji, Kim Minah, Kwon Jun Soo

机构信息

Department of Neuropsychiatry, Seoul National University Hospital, Seoul, Republic of Korea.

Department of Psychiatry, Seoul National University College of Medicine, Seoul, Republic of Korea.

出版信息

Eur J Neurosci. 2025 Sep;62(5):e70256. doi: 10.1111/ejn.70256.

Abstract

Duration-deviant mismatch negativity has been investigated as a potential biomarker for predicting early psychosis clinical outcomes. Although progressive mismatch negativity changes have been linked to neurodegeneration and cognitive decline after psychosis onset, it is unclear whether similar changes occur in patients at clinical high risk for psychosis. Therefore, we examined longitudinal mismatch negativity changes and their associations with cognition and functioning in 24 clinical high risk for psychosis individuals and 22 healthy controls. Participants underwent duration-deviant mismatch negativity recordings at baseline and the 1-2-year follow-up. Neurocognitive functioning was assessed via Trail Making Test parts A and B, and general functioning was measured with the Global Assessment of Functioning scale. Group differences in mismatch negativity amplitude change over time were evaluated using repeated-measures analysis of covariance, and its associations with cognitive and functional changes were assessed via Spearman correlations. Compared with healthy controls, individuals at clinical high risk for psychosis had significantly reduced mismatch negativity amplitudes at the FCz electrode site at baseline. However, there was no significant group-by-time interaction in mismatch negativity amplitude, nor were its changes significantly correlated with neurocognitive or general functioning changes, suggesting that progressive changes in duration-deviant mismatch negativity may not occur prior to psychosis onset in individuals at clinical high risk for psychosis. Given the heterogeneous outcomes in the clinical high risk for psychosis population, larger samples and longer follow-up durations are needed to elucidate the clinical significance of duration-deviant mismatch negativity in this group.

摘要

持续时间偏差失配负波已被作为预测早期精神病临床结局的潜在生物标志物进行研究。尽管精神病发作后失配负波的渐进性变化与神经退行性变和认知衰退有关,但尚不清楚在临床高危精神病患者中是否会出现类似变化。因此,我们研究了24名临床高危精神病个体和22名健康对照者失配负波的纵向变化及其与认知和功能的关系。参与者在基线和1-2年随访时进行了持续时间偏差失配负波记录。通过连线测验A和B部分评估神经认知功能,并用功能总体评定量表测量总体功能。使用重复测量协方差分析评估失配负波幅度随时间的组间差异,并通过斯皮尔曼相关性评估其与认知和功能变化的关联。与健康对照相比,临床高危精神病个体在基线时FCz电极部位的失配负波幅度显著降低。然而,失配负波幅度没有显著的组×时间交互作用,其变化也与神经认知或总体功能变化无显著相关性,这表明在临床高危精神病个体中,持续时间偏差失配负波的渐进性变化可能在精神病发作之前不会出现。鉴于临床高危精神病群体的结果存在异质性,需要更大的样本量和更长的随访时间来阐明该组中持续时间偏差失配负波的临床意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/362f/12433931/d8b2ae0b6dd8/EJN-62-0-g002.jpg

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