新冠肺炎后大脑结构变化及其与认知障碍的关系

IF 4.1 Q1 CLINICAL NEUROLOGY
Brain communications Pub Date : 2025-02-12 eCollection Date: 2025-01-01 DOI:10.1093/braincomms/fcaf070
Laura Pacheco-Jaime, Carla Garcia-Vicente, Mar Ariza, Neus Cano, Maite Garolera, Lourdes Carreras-Vidal, Ignacio Roura, Clara Capdevila-Lacasa, Javier Oltra, Jèssica Pardo, Cristina Martín-Barceló, Anna Campabadal, Roser Sala-Llonch, Núria Bargalló, Cristian Barrué, Javier Bejar, Claudio U Cortés, Carme Junqué, Bàrbara Segura
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引用次数: 0

摘要

据估计,SARS-CoV-2感染者中约有4%会被诊断为后冠状病毒感染。先前的研究已经证明,感染者存在认知功能障碍和大脑结构变化;然而,新冠肺炎后结构变化与认知变化之间的关系尚不清楚。因此,这项工作的目的是研究感染近2年后covid后患者的大脑结构变化及其与患者认知障碍的可能关系。此外,还探讨了与血液生物标志物和临床变量的关系。来自Nautilus项目(ClinicalTrials.gov id: NCT05307549和NCT05307575)的128名新冠肺炎后患者和37名未感染的健康对照者接受了结构脑磁共振成像和综合神经心理学评估。66名covid后参与者的子样本也进行了血液提取,以获得血液生物标志物的水平。使用FreeSurfer (v7.1)获取皮质厚度和皮质下体积并进行分析。使用FMRIB Software Library软件(v6.0.4)进行基于灰质体素的分析,研究微结构白质完整性。与健康对照组相比,新冠肺炎后患者在工作记忆和言语记忆、处理速度、言语流畅性和执行功能方面的表现明显较差。此外,新冠肺炎后患者右额上回和右吻侧额中回皮层厚度增加,与工作记忆表现呈负相关。弥散张量成像数据显示,患者的右上纵束、胼胝体的脾和膝、右钩叶束和大钳的各向异性分数较低,与主观记忆失败呈负相关。血液生物标志物没有发现差异。一旦根据患者的认知状态对其进行分类,与归类为非认知改变的患者相比,covid后临床认知改变的患者皮层厚度增加。总之,我们的研究表明,在近两年的感染后,大脑灰质和白质的变化与这种情况有关,并在一定程度上解释了长期的认知后遗症。这些发现强调了长期监测这些高危人群的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Structural brain changes in post-COVID condition and its relationship with cognitive impairment.

It has been estimated that ∼4% of individuals infected with SARS-CoV-2 will be diagnosed with post-COVID condition. Previous studies have evidenced the presence of cognitive dysfunction and structural brain changes in infected individuals; however, the relationship between structural changes and cognitive alterations in post-COVID condition is still not clear. Consequently, the aim of this work is to study structural brain alterations in post-COVID condition patients after almost 2 years of infection and their likely relationship with patients' cognitive impairment. Additionally, the association with blood biomarkers and clinical variables was also explored. One hundred and twenty-eight individuals with post-COVID condition and 37 non-infected healthy controls from the Nautilus Project (ClinicalTrials.gov IDs: NCT05307549 and NCT05307575) underwent structural brain magnetic resonance imaging and a comprehensive neuropsychological assessment. A subsample of 66 post-COVID participants also underwent blood extraction to obtain levels of blood biomarkers. Cortical thickness and subcortical volumes were obtained and analysed using FreeSurfer (v7.1). FMRIB Software Library software (v6.0.4) was used to perform grey matter voxel-based analysis and to study microstructural white matter integrity. Patients with post-COVID performed significantly worse in working and verbal memory, processing speed, verbal fluency and executive functions, compared to healthy controls. Moreover, patients with post-COVID showed increased cortical thickness in the right superior frontal and the right rostral middle frontal gyri that negatively correlated with working memory performance. Diffusion tensor imaging data showed lower fractional anisotropy in patients in the right superior longitudinal fasciculus, the splenium and genu of the corpus callosum, the right uncinate fasciculus and the forceps major, that negatively correlated with subjective memory failures. No differences in blood biomarkers were found. Once patients were classified according to their cognitive status, post-COVID clinically cognitively altered presented increased cortical thickness compared to those classified as non-cognitively altered. In conclusion, our study showed that grey and white matter brain changes are relevant in this condition after almost 2 years of infection and partly explain long-term cognitive sequelae. These findings underscore the critical importance of monitoring this at-risk population over time.

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