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在美国健康与退休研究中,种族/族裔与胱抑素C循环血液水平对认知状态的交互作用及中介效应分解

Decomposing interaction and mediating effects of race/ethnicity and circulating blood levels of cystatin C on cognitive status in the United States health and retirement study.

作者信息

Higgins Tejera César, Ware Erin B, Kobayashi Lindsay C, Fu Mingzhou, Hicken Margaret, Zawistowski Matthew, Mukherjee Bhramar, Bakulski Kelly M

机构信息

Department of Epidemiology, School of Public Health, University of Michigan, Ann Arbor, MI, United States.

Institute for Social Research, University of Michigan, Ann Arbor, MI, United States.

出版信息

Front Hum Neurosci. 2023 Jun 1;17:1052435. doi: 10.3389/fnhum.2023.1052435. eCollection 2023.

Abstract

BACKGROUND AND OBJECTIVES

Elevated circulating cystatin C is associated with cognitive impairment in non-Hispanic Whites, but its role in racial disparities in dementia is understudied. In a nationally representative sample of older non-Hispanic White, non-Hispanic Black, and Hispanic adults in the United States, we use mediation-interaction analysis to understand how racial disparities in the cystatin C physiological pathway may contribute to racial disparities in prevalent dementia.

METHODS

In a pooled cross-sectional sample of the Health and Retirement Study ( = 9,923), we employed Poisson regression to estimate prevalence ratios and to test the relationship between elevated cystatin C (>1.24 vs. ≤1.24 mg/L) and impaired cognition, adjusted for demographics, behavioral risk factors, other biomarkers, and chronic conditions. Self-reported racialized social categories were a proxy measure for exposure to racism. We calculated additive interaction measures and conducted four-way mediation-interaction decomposition analysis to test the moderating effect of race/ethnicity and mediating effect of cystatin C on the racial disparity.

RESULTS

Overall, elevated cystatin C was associated with dementia (prevalence ratio [PR] = 1.2; 95% CI: 1.0, 1.5). Among non-Hispanic Black relative to non-Hispanic White participants, the relative excess risk due to interaction was 0.7 (95% CI: -0.1, 2.4), the attributable proportion was 0.1 (95% CI: -0.2, 0.4), and the synergy index was 1.1 (95% CI: 0.8, 1.8) in a fully adjusted model. Elevated cystatin C was estimated to account for 2% (95% CI: -0, 4%) for the racial disparity in prevalent dementia, and the interaction accounted for 8% (95% CI: -5, 22%). Analyses for Hispanic relative to non-white participants suggested moderation by race/ethnicity, but not mediation.

DISCUSSION

Elevated cystatin C was associated with dementia prevalence. Our mediation-interaction decomposition analysis suggested that the effect of elevated cystatin C on the racial disparity might be moderated by race/ethnicity, which indicates that the racialization process affects not only the distribution of circulating cystatin C across minoritized racial groups, but also the strength of association between the biomarker and dementia prevalence. These results provide evidence that cystatin C is associated with adverse brain health and this effect is larger than expected for individuals racialized as minorities had they been racialized and treated as non-Hispanic White.

摘要

背景与目的

循环胱抑素C升高与非西班牙裔白人的认知障碍有关,但其在痴呆症种族差异中的作用尚未得到充分研究。在美国具有全国代表性的老年非西班牙裔白人、非西班牙裔黑人及西班牙裔成年人样本中,我们使用中介-交互分析来了解胱抑素C生理途径中的种族差异如何导致普遍痴呆症中的种族差异。

方法

在健康与退休研究的汇总横断面样本(n = 9923)中,我们采用泊松回归来估计患病率比,并检验胱抑素C升高(>1.24 vs.≤1.24 mg/L)与认知障碍之间的关系,对人口统计学、行为风险因素、其他生物标志物和慢性病进行了调整。自我报告的种族化社会类别是衡量遭受种族主义的替代指标。我们计算了相加交互作用指标,并进行了四向中介-交互作用分解分析,以检验种族/族裔的调节作用和胱抑素C对种族差异的中介作用。

结果

总体而言,胱抑素C升高与痴呆症有关(患病率比[PR]=1.2;95%CI:1.0,1.5)。在非西班牙裔黑人相对于非西班牙裔白人参与者中,在完全调整模型中,交互作用导致的相对超额风险为0.7(95%CI:-0.1,2.4),归因比例为0.1(95%CI:-0.2,0.4),协同指数为1.1(95%CI:0.8,1.8)。估计胱抑素C升高占普遍痴呆症种族差异的2%(95%CI:-0,4%),交互作用占8%(95%CI:-5,22%)。对西班牙裔相对于非白人参与者的分析表明存在种族/族裔调节作用,但不存在中介作用。

讨论

胱抑素C升高与痴呆症患病率有关。我们的中介-交互作用分解分析表明,胱抑素C升高对种族差异的影响可能受种族/族裔调节,这表明种族化过程不仅影响循环胱抑素C在少数族裔群体中的分布,还影响生物标志物与痴呆症患病率之间关联的强度。这些结果提供了证据,表明胱抑素C与不良脑健康有关,并且对于被种族化为少数族裔的个体来说,这种影响比将他们种族化为非西班牙裔白人时预期的更大。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c17/10267311/d2fb43e998d8/fnhum-17-1052435-g001.jpg

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