Department of Neurology, Emory University School of Medicine, Atlanta, Georgia.
Department of Neurology, University of Texas Southwestern, Dallas.
JAMA Netw Open. 2022 Oct 3;5(10):e2235068. doi: 10.1001/jamanetworkopen.2022.35068.
Differences in cerebrospinal fluid (CSF) tau Alzheimer dementia (AD) biomarkers by self-identified race have been observed in prior studies. More recently, plasma biomarkers have been gaining recognition, but whether they exhibit similar differences is unclear. Furthermore, the underlying explanation for these differences in AD biomarkers is still unexplored.
To investigate differences in plasma biomarkers by race and genetic ancestry and explore potential underlying explanations for these differences.
DESIGN, SETTING, AND PARTICIPANTS: This cross-sectional study used participant data from the Brain, Stress, Hypertension, and Aging Research Program (B-SHARP), an observational study conducted in the greater Atlanta metropolitan area. Participants were enrolled from March 1, 2016, to January 1, 2020.
Main outcomes were plasma and CSF amyloid-β (Aβ) 42, Aβ40, phosphorylated tau181 (p-tau181), and neurofilament light. General linear models were used for key comparisons.
Main independent variables were self-identified race and genetic ancestry. Additional variables were cardiovascular factors, APOE4, educational attainment, Area Deprivation Index, and C-reactive protein (reflecting systemic inflammation state).
This analysis included 617 participants (mean [SD] age, 66 [7.9] years; 300 [49%] African American and 317 [51%] White; 429 [70%] with mild cognitive impairment). On the basis of self-reported race, plasma levels of Aβ42 (adjusted mean difference, -1.20 pg/mL; 95% CI, -2.33 to -0.07 pg/mL), Aβ40 (adjusted mean difference, -37.78 pg/mL; 95% CI, -60.16 to -15.39 pg/mL), p-tau181 (adjusted mean difference, -4.66 pg/mL; 95% CI, -7.05 to -1.90 pg/mL), and neurofilament light (adjusted mean difference, -1.58; 95% CI, -2.83 to -0.19 pg/mL) were consistently lower in African American individuals after adjusting for demographic characteristics, educational attainment, cognition, APOE4, and cardiovascular factors. A similar pattern was observed in the CSF biomarkers except for Aβ42 and Aβ40. Although unadjusted analyses revealed an association between these biomarkers and African ancestry, these associations were not significant after adjusting for the same covariates. Differences by self-reported race were not explained by varied cardiovascular risk factors, C-reactive protein, educational attainment, or Area Deprivation Index.
In this cross-sectional study of plasma biomarkers by race and genetic ancestry, the results indicated that plasma p-tau181, Aβ40, and NFL were lower in African American individuals based on self-reported race but not genetic ancestry. These differences were not explained by cardiovascular risks or clinical stage differences. These racial differences should be considered in clinical interpretations and clinical trial screenings to avoid an additional increase in underrepresentation of African American individuals in AD trials.
先前的研究已经观察到,在自我认定的种族之间,脑脊液(CSF)tau 阿尔茨海默病(AD)生物标志物存在差异。最近,血浆生物标志物也越来越受到认可,但它们是否存在类似的差异尚不清楚。此外,这些 AD 生物标志物差异的潜在解释仍未得到探索。
研究种族和遗传血统对血浆生物标志物的影响,并探讨这些差异的潜在解释。
设计、地点和参与者:本横断面研究使用了来自 Brain, Stress, Hypertension, and Aging Research Program (B-SHARP) 的参与者数据,该研究是在亚特兰大大都市区进行的一项观察性研究。参与者于 2016 年 3 月 1 日至 2020 年 1 月 1 日入组。
主要结局为血浆和 CSF 淀粉样蛋白-β(Aβ)42、Aβ40、磷酸化 tau181(p-tau181)和神经丝轻链。主要比较采用一般线性模型。
主要的独立变量是自我认定的种族和遗传血统。其他变量包括心血管因素、APOE4、教育程度、区域剥夺指数和 C 反应蛋白(反映全身炎症状态)。
本分析纳入了 617 名参与者(平均[标准差]年龄 66[7.9]岁;300[49%]为非裔美国人,317[51%]为白人;429[70%]为轻度认知障碍)。基于自我报告的种族,血浆 Aβ42(调整后的平均差异,-1.20 pg/mL;95%CI,-2.33 至-0.07 pg/mL)、Aβ40(调整后的平均差异,-37.78 pg/mL;95%CI,-60.16 至-15.39 pg/mL)、p-tau181(调整后的平均差异,-4.66 pg/mL;95%CI,-7.05 至-1.90 pg/mL)和神经丝轻链(调整后的平均差异,-1.58;95%CI,-2.83 至-0.19 pg/mL)在调整人口统计学特征、教育程度、认知、APOE4 和心血管因素后,非裔美国人的水平持续较低。CSF 生物标志物中也观察到类似的模式,但除了 Aβ42 和 Aβ40 之外。尽管未调整的分析显示这些生物标志物与非洲血统之间存在关联,但在调整相同协变量后,这些关联并不显著。基于自我报告的种族的差异不能用不同的心血管风险因素、C 反应蛋白、教育程度或区域剥夺指数来解释。
在这项关于种族和遗传血统的血浆生物标志物的横断面研究中,结果表明,基于自我报告的种族,非裔美国人的血浆 p-tau181、Aβ40 和 NFL 水平较低,但不是遗传血统。这些差异不能用心血管风险或临床阶段差异来解释。在临床解释和临床试验筛选中应考虑这些种族差异,以避免 AD 试验中非洲裔美国人的代表性进一步不足。
