Associations between metabolic syndrome and markers of brain pathology: the role of sex- differences

IF 1.9 Q3 CLINICAL NEUROLOGY
Anna Marseglia , Alexandra Cooper , Lina Ryden , Silke Kern , Sara Shams , Olof Lindberg , Kaj Blennow , Henrik Zetterberg , Anna Zettergren , Ingmar Skoog , Eric Westman , Henrik Zetterberg , Anna Zettergren , Ingmar Skoog , Eric Westman
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引用次数: 0

Abstract

Introduction

Cardiovascular and metabolic disorders rarely occur alone in old age but often cluster together in the so-called metabolic syndrome (MetS). While individual components of MetS, such as obesity, hypertension, and diabetes, have been linked to dementia and brain atrophy, their combined impact on cognitive and brain aging remains poorly explored. Our current study aims to investigate the relationship between MetS and markers of neurodegenerative and cerebrovascular pathologies while also considering potential differences between sexes.

Methods

We included 741 cognitively intact septuagenarians from the Gothenburg H70-Birth cohort 1944 with available brain MRI (286 had cerebrospinal fluid [CSF] sampling). MetS was defined by standard criteria (at least three among adiposity, raised blood pressure, blood glucose, reduced HDL-cholesterol, elevated triglycerides). MRI markers of brain pathology included overall (mean cortical thickness) and Alzheimer's disease (AD; average cortical thickness in signature areas) neurodegeneration, cerebral small vessel disease (SVD; markers such as white matter hyperintensity, lacunes, microbleeds, and perivascular spaces, and SVD score) and DTI's white- matter microstructural changes (fractional anisotropy). CSF biomarkers included t-tau, neurofilament light, neurogranin (overall neurodegeneration), Aβ42 and p-tau (AD), and CSF/serum albumin ratio (blood-brain barrier integrity). Analyses included regression models and stratification by sex.

Results

Overall, 410 participants (53%, n=196 women) had MetS. MetS was associated with increased odds of overall (OR=2.0, 95%CI 1.4–2.9) and AD-related (OR=1.8, 95%CI 1.4–2.6) neurodegeneration, high SVD burden (presence of ≥3 SVD compared to none: OR=2.1, 95%CI 1.1–4.3), and white-matter microstructural changes. Within the SVD markers, MetS was particularly related to white matter hyperintensities, lacunes, and perivascular spaces in basal ganglia. Furthermore, MetS was associated with alterations of blood-brain barrier integrity in the CSF subsample. Sex differences showed increased SVD burden in men with MetS, especially enlarged perivascular spaces (OR=2.9, 95%CI 1.7–5.0), while no differences were observed in women. No associations were detected with amyloid and tau.

Discussion

MetS in late life is linked to neurodegenerative and cerebrovascular pathologies, with SVD more prominent in men with MetS, but not in women.

代谢综合征与脑病理学标志物之间的关系:性别差异的作用
导言:心血管疾病和代谢紊乱很少单独发生在老年人身上,而是经常聚集在一起,形成所谓的代谢综合征(MetS)。虽然肥胖、高血压和糖尿病等代谢综合征的单个成分与痴呆症和脑萎缩有关,但它们对认知和大脑老化的综合影响仍未得到充分探讨。我们目前的研究旨在调查 MetS 与神经退行性病变和脑血管病变标志物之间的关系,同时考虑性别之间的潜在差异。方法我们纳入了哥德堡 H70-Birth 队列 1944 中 741 名认知功能完好的七旬老人,他们都有脑部 MRI(286 人有脑脊液 [CSF] 采样)。MetS按照标准定义(脂肪过多、血压升高、血糖升高、高密度脂蛋白胆固醇降低、甘油三酯升高中至少有三项)。脑部病理的 MRI 标志物包括总体(平均皮质厚度)和阿尔茨海默病(AD;特征区域的平均皮质厚度)神经变性、脑小血管病(SVD;标志物如白质高密度、裂隙、微出血、血管周围间隙和 SVD 评分)以及 DTI 的白质微结构变化(分数各向异性)。CSF生物标记物包括t-tau、神经丝光、神经粒蛋白(整体神经变性)、Aβ42和p-tau(AD)以及CSF/血清白蛋白比值(血脑屏障完整性)。分析包括回归模型和性别分层。MetS与总体(OR=2.0,95%CI 1.4-2.9)和AD相关(OR=1.8,95%CI 1.4-2.6)神经变性、高SVD负担(存在≥3种SVD而无SVD:OR=2.1,95%CI 1.1-4.3)和白质微结构变化的几率增加有关。在SVD标记物中,MetS与基底节的白质高密度、裂隙和血管周围间隙尤为相关。此外,MetS还与CSF子样本中血脑屏障完整性的改变有关。性别差异显示,患有 MetS 的男性 SVD 负荷增加,尤其是血管周围间隙增大(OR=2.9,95%CI 1.7-5.0),而女性则无差异。讨论晚年MetS与神经退行性病变和脑血管病变有关,SVD在患有MetS的男性中更为突出,但在女性中并不明显。
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来源期刊
Cerebral circulation - cognition and behavior
Cerebral circulation - cognition and behavior Neurology, Clinical Neurology
CiteScore
2.00
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审稿时长
14 weeks
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