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自我认定为黑人/非裔美国人和白人个体的血浆Aβ42/40的基线水平及纵向变化率。

Baseline levels and longitudinal rates of change in plasma Aβ42/40 among self-identified Black/African American and White individuals.

作者信息

Xiong Chengjie, Schindler Suzanne, Luo Jingqin, Morris John, Bateman Randall, Holtzman David, Cruchaga Carlos, Babulal Ganesh, Henson Rachel, Benzinger Tammie, Bui Quoc, Agboola Folasade, Grant Elizabeth, Emily Gremminger, Moulder Krista, Geldmacher David, Clay Olivio, Roberson Erik, Murchison Charles, Wolk David, Shaw Leslie

机构信息

Washington University in St. Louis.

Washington University School of Medicine.

出版信息

Res Sq. 2024 Jan 8:rs.3.rs-3783571. doi: 10.21203/rs.3.rs-3783571/v1.

Abstract

OBJECTIVE

The use of blood-based biomarkers of Alzheimer disease (AD) may facilitate access to biomarker testing of groups that have been historically under-represented in research. We evaluated whether plasma Aβ42/40 has similar or different baseline levels and longitudinal rates of change in participants racialized as Black or White.

METHODS

The Study of Race to Understand Alzheimer Biomarkers (SORTOUT-AB) is a multi-center longitudinal study to evaluate for potential differences in AD biomarkers between individuals racialized as Black or White. Plasma samples collected at three AD Research Centers (Washington University, University of Pennsylvania, and University of Alabama-Birmingham) underwent analysis with CN Diagnostics' PrecivityAD blood test for Aβ42 and Aβ40. General linear mixed effects models were used to estimate the baseline levels and rates of longitudinal change for plasma Aβ measures in both racial groups. Analyses also examined whether dementia status, age, sex, education, 4 carrier status, medical comorbidities, or fasting status modified potential racial differences.

RESULTS

Of the 324 Black and 1,547 White participants, there were 158 Black and 759 White participants with plasma Aβ measures from at least two longitudinal samples over a mean interval of 6.62 years. At baseline, the group of Black participants had lower levels of plasma Aβ40 but similar levels of plasma Aβ42 as compared to the group of White participants. As a result, baseline plasma Aβ42/40 levels were higher in the Black group than the White group, consistent with the Black group having lower levels of amyloid pathology. Racial differences in plasma Aβ42/40 were not modified by age, sex, education, 4 carrier status, medical conditions (hypertension and diabetes), or fasting status. Despite differences in baseline levels, the Black and White groups had a similar longitudinal rate of change in plasma Aβ42/40.

INTERPRETATION

Black individuals participating in AD research studies had a higher mean level of plasma Aβ42/40, consistent with a lower level of amyloid pathology, which, if confirmed, may imply a lower proportion of Black individuals being eligible for AD clinical trials in which the presence of amyloid is a prerequisite. However, there was no significant racial difference in the rate of change in plasma Aβ42/40, suggesting that amyloid pathology accumulates similarly across racialized groups.

摘要

目的

使用基于血液的阿尔茨海默病(AD)生物标志物可能有助于对研究中历史上代表性不足的群体进行生物标志物检测。我们评估了在按种族划分为黑人或白人的参与者中,血浆Aβ42/40是否具有相似或不同的基线水平和纵向变化率。

方法

了解阿尔茨海默病生物标志物的种族研究(SORTOUT - AB)是一项多中心纵向研究,旨在评估按种族划分为黑人或白人的个体之间AD生物标志物的潜在差异。在三个AD研究中心(华盛顿大学、宾夕法尼亚大学和阿拉巴马大学伯明翰分校)采集的血浆样本,使用CN诊断公司的PrecivityAD血液检测法对Aβ42和Aβ40进行分析。采用一般线性混合效应模型来估计两个种族组中血浆Aβ指标的基线水平和纵向变化率。分析还检查了痴呆状态、年龄、性别、教育程度、4基因携带者状态、合并症或禁食状态是否会改变潜在的种族差异。

结果

在324名黑人参与者和1547名白人参与者中,有158名黑人和759名白人参与者在平均6.62年的时间间隔内,至少有两个纵向样本的血浆Aβ测量值。基线时,与白人参与者组相比,黑人参与者组的血浆Aβ40水平较低,但血浆Aβ42水平相似。因此,黑人组的基线血浆Aβ42/40水平高于白人组,这与黑人组的淀粉样蛋白病理学水平较低一致。血浆Aβ42/40的种族差异不受年龄、性别、教育程度、4基因携带者状态、医疗状况(高血压和糖尿病)或禁食状态的影响。尽管基线水平存在差异,但黑人和白人组血浆Aβ42/40的纵向变化率相似。

解读

参与AD研究的黑人个体血浆Aβ42/40的平均水平较高,这与较低的淀粉样蛋白病理学水平一致,如果得到证实,这可能意味着有资格参加以淀粉样蛋白存在为前提条件的AD临床试验的黑人个体比例较低。然而,血浆Aβ42/40的变化率在种族之间没有显著差异,这表明淀粉样蛋白病理学在不同种族群体中的积累情况相似。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c283/10802715/e9b634c517a7/nihpp-rs3783571v1-f0001.jpg

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