Relation Between Markers of Systemic Inflammation, White Matter Lesions, and Cognitive Performance in Late Adulthood

IF 13 1区医学 Q1 CLINICAL NEUROLOGY

Alzheimer's & Dementia Pub Date : 2025-01-09 DOI:10.1002/alz.087429

Shivangi Jain, Alina Lesnovskaya, Lu Wan, Cristina Molina‐Hidalgo, Haiqing Huang, Anna Marsland, George Grove, Lauren Oberlin, Chaeryon Kang, Arthur Kramer, Charles Hillman, Edward McAuley, Jeffrey M Burns, Eric D Vidoni, Brad Sutton, Kirk I. Erickson

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引用次数: 0

Abstract

BackgroundAging is associated with heightened systemic inflammation, decline in selective aspects of cognition, and an increase in white matter lesions (WMLs). Both WMLs and systemic inflammation have been related to cognition. However, it is not clear how they interdependently relate to cognitive aging. In this study we examined whether WMLs mediate the relation between markers of systemic inflammation and cognition in late adulthood.MethodBaseline data from the randomized clinical trial “Investigating Gains in Neurocognition in an Intervention Trial of Exercise” (IGNITE) were used, which included 598 healthy older adults (mean age=69.9±3.75 years). Interleukin 6 (IL‐6) and Tumor Necrosis Factor Alpha (TNF‐α) were included as markers of systemic inflammation. A confirmatory factor analysis of cognitive performance resulted in factors measuring episodic memory (EM), processing speed (PS), working memory (WM), attentional control (AC), and visuospatial function (VF). WML volumes were computed from FLAIR and T1 scans using UBO detector. Mediation models were run with age, sex, years of education, and study site included as covariates.ResultHigher levels of IL‐6 were associated with more WMLs (b = 0.12, p < 0.001) as well as lower scores on all cognitive factors (all p < 0.03). In contrast, higher levels of TNF‐ α were associated with more WMLs (b = 0.10, p < 0.05) but not with any of the cognitive measures (all p > 0.3). More WMLs were associated with poorer PS, WM, AC, and VF (all p < 0.03), but not EM (all p > 0.05). Further, associations between IL‐6 and measures of PS, WM, AC, and VF were statistically mediated by WMLs (all b = ‐0.01, all p < 0.05).ConclusionThese findings suggest that markers of systemic inflammation might lead to poorer cognitive performance by impacting WMLs. The differences between IL‐6 and TNF‐α with cognition highlight the need for more research to understand how different cytokine pathways relate to cognition. Our results are important for building a mechanistic framework to understand the interplay between inflammation, WMLs, and cognition and could inform the development of targeted interventions focusing on regulating cytokines to support brain health and cognitive aging.

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成年后期全身性炎症、白质病变与认知表现之间的关系

背景衰老与全身性炎症加剧、认知选择性方面的下降和白质病变（WMLs）的增加有关。脑损伤和全身性炎症都与认知有关。然而，目前尚不清楚它们是如何相互依赖地与认知衰老联系在一起的。在这项研究中，我们研究了脑白质损伤是否介导了成年后期全身性炎症标志物与认知之间的关系。方法采用随机临床试验“研究运动干预试验中神经认知的获益”（IGNITE）的基线数据，纳入598名健康老年人（平均年龄=69.9±3.75岁）。白细胞介素6 （IL - 6）和肿瘤坏死因子α (TNF - α)作为全身性炎症的标志物。认知表现的验证性因素分析包括情景记忆（EM）、加工速度（PS）、工作记忆（WM）、注意控制（AC）和视觉空间功能（VF）。使用UBO检测器从FLAIR和T1扫描中计算WML体积。以年龄、性别、受教育年限和研究地点作为协变量运行中介模型。结果白细胞介素- 6水平与WMLs发生率相关(b = 0.12, p <；0.001)，所有认知因素的得分都较低(p <；0.03)。相反，较高水平的TNF‐α与更多的脑白质损伤相关(b = 0.10, p <；0.05)，但与任何认知测试都没有关系(所有p >；0.3)。WMLs越多，PS、WM、AC和VF越差(p <；0.03)，但不包括EM(全部p >；0.05)。此外，IL - 6与PS、WM、AC和VF之间的关联在统计学上由wml介导(均为b =‐0.01，均为p <；0.05)。结论全身性炎症标志物可能通过影响脑损伤导致认知能力下降。IL - 6和TNF - α与认知之间的差异强调了需要更多的研究来了解不同的细胞因子途径如何与认知相关。我们的研究结果对于建立一个机制框架来理解炎症、脑白质损伤和认知之间的相互作用具有重要意义，并且可以为有针对性的干预措施的发展提供信息，这些干预措施侧重于调节细胞因子，以支持大脑健康和认知衰老。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Alzheimer's & Dementia 医学-临床神经学

CiteScore

14.50

自引率

5.00%

发文量

299

审稿时长

3 months

期刊介绍： Alzheimer's & Dementia is a peer-reviewed journal that aims to bridge knowledge gaps in dementia research by covering the entire spectrum, from basic science to clinical trials to social and behavioral investigations. It provides a platform for rapid communication of new findings and ideas, optimal translation of research into practical applications, increasing knowledge across diverse disciplines for early detection, diagnosis, and intervention, and identifying promising new research directions. In July 2008, Alzheimer's & Dementia was accepted for indexing by MEDLINE, recognizing its scientific merit and contribution to Alzheimer's research.