晚年对心血管疾病风险的易感性是否与轻度认知障碍老年人的纵向tau蛋白积累有关?
Is late-life vulnerability to cardiovascular disease risk associated with longitudinal tau accumulation in older adults with mild cognitive impairment?
作者信息
Dratva M A, Diaz J M, Thomas M L, Shen Q, Tsiknia A A, Rostowsky K A, Sundermann E E, Banks S J
机构信息
Department of Neurosciences, University of California, San Diego, La Jolla, CA, USA.
Department of Psychology, Colorado State University, Fort Collins, CO, USA.
出版信息
JAR Life. 2025 Feb 18;14:100001. doi: 10.1016/j.jarlif.2025.100001. eCollection 2025.
BACKGROUND
Older females have higher Alzheimer's Disease (AD) risk and tau burden, especially in early disease stages, compared to males. Overlapping cardiovascular disease (CVD) and dementia risk factors, like the apolipoprotein (APOE)-ε4 allele, show mixed sex-specific results. We previously found that late-life CVD risk related more strongly to tau at a single timepoint in cognitively normal, older female APOE-ε4 carriers than in males.
OBJECTIVES
Do composite and component CVD risk factors explain sex differences in tau accumulation in older adults with mild cognitive impairment (MCI) and underlying amyloid-beta (Aβ) pathology?
DESIGN
Longitudinal analysis in the Alzheimer's Disease Neuroimaging Initiative (ADNI) cohort.
SETTING
ADNI is a multi-site longitudinal study across the United States and Canada.
PARTICIPANTS
= 52 older adults (aged 60-90), designated as both Aβ-positive and MCI.
MEASUREMENTS
CVD risk was measured by body mass index (BMI) and FRS, which includes age, systolic blood pressure (BP), high-density lipoprotein (HDL), total cholesterol, hypertension treatment, smoking, and diabetes. Regional standardized uptake value ratios (SUVRs) were extracted at each tau-PET timepoint. Composite SUVRs for Braak34 and Braak56 were calculated. Statistical models examined the separate and interactive effects of sex and APOE-ε4 on tau accumulation, and moderating effects of FRS, its components, or BMI, on tau accumulation.
RESULTS
Females accumulated more tau than males in bilateral Braak34 and right Braak56, while APOE-ε4 carriers trended toward more tau accumulation in left Braak56. FRS and its components did not relate to tau accumulation, nor influence sex effects, although they attenuated APOE-ε4 effects. In left Braak56, higher baseline BMI in males showed a trend toward greater tau accumulation.
CONCLUSIONS
In MCI and Aβ-positive older adults, females accumulated more tau than males, and late-life vascular risk did not explain this relationship. Higher BMI related to more tau accumulation in males only, suggesting sex-specific vulnerability to BMI on brain health. Although replication in larger and more representative cohorts is needed, these findings corroborate accelerated tau progression in older females, independent of CVD risk, and suggest that vascular health has limited influence on tau progression once AD pathology is established in the brain.
背景
与男性相比,老年女性患阿尔茨海默病(AD)的风险和tau蛋白负担更高,尤其是在疾病早期阶段。重叠的心血管疾病(CVD)和痴呆风险因素,如载脂蛋白(APOE)-ε4等位基因,显示出不同的性别特异性结果。我们之前发现,在认知正常的老年女性APOE-ε4携带者中,晚年CVD风险在单个时间点与tau蛋白的相关性比男性更强。
目的
综合和单项CVD风险因素是否能解释轻度认知障碍(MCI)且存在淀粉样蛋白-β(Aβ)病理改变的老年人中tau蛋白积累的性别差异?
设计
对阿尔茨海默病神经影像学倡议(ADNI)队列进行纵向分析。
背景
ADNI是一项在美国和加拿大开展的多中心纵向研究。
参与者
52名老年人(年龄在60 - 90岁之间),被判定为Aβ阳性且患有MCI。
测量指标
通过体重指数(BMI)和弗雷明汉心脏研究风险评分(FRS)来衡量CVD风险,FRS包括年龄、收缩压(BP)、高密度脂蛋白(HDL)、总胆固醇、高血压治疗情况、吸烟状况和糖尿病。在每个tau蛋白正电子发射断层扫描(PET)时间点提取区域标准化摄取值比率(SUVRs)。计算Braak34和Braak56的综合SUVRs。统计模型检验了性别和APOE-ε4对tau蛋白积累的单独及交互作用,以及FRS及其组成部分或BMI对tau蛋白积累的调节作用。
结果
在双侧Braak34和右侧Braak56区域,女性比男性积累了更多的tau蛋白,而APOE-ε4携带者在左侧Braak56区域有更多tau蛋白积累的趋势。FRS及其组成部分与tau蛋白积累无关,也不影响性别效应,尽管它们减弱了APOE-ε4的效应。在左侧Braak56区域,男性较高的基线BMI显示出tau蛋白积累更多的趋势。
结论
在MCI且Aβ阳性的老年人中,女性比男性积累了更多的tau蛋白,且晚年血管风险无法解释这种关系。较高的BMI仅与男性更多的tau蛋白积累相关,表明在脑健康方面男性对BMI具有性别特异性易感性。尽管需要在更大且更具代表性的队列中进行重复验证,但这些发现证实了老年女性中tau蛋白进展加速,与CVD风险无关,并表明一旦大脑中确立了AD病理,血管健康对tau蛋白进展的影响有限。
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