Alzheimer's disease biomarkers in Black and non‐Hispanic White cohorts: A contextualized review of the evidence

Gleason, Carey E.; Zuelsdorff, Megan; Gooding, Diane C.; Kind, Amy J H; Johnson, Adrienne L.; James, Taryn T.; Lambrou, Nickolas H.; Wyman, Mary F.; Ketchum, Fred B.; Gee, Alexander; Johnson, Sterling C.; Bendlin, Barbara B.; Zetterberg, Henrik

doi:10.1002/alz.12511

Cited by 40 publications

(57 citation statements)

References 112 publications

(258 reference statements)

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“…Data has shown that biomarker changes in AD can vary between Blacks and Whites, and similar biomarker profiles can be associated with divergent cognitive function. 37 To date, it is unknown how frequently biomarker testing of asymptomatic persons is pursued in clinical practice. Surveys conducted prior to the approval of amyloid PET scans for clinical use found that a majority of dementia specialists planned to use them to identify asymptomatic persons at risk for AD dementia, 38 while others would be reluctant to share results for fear of negative psychosocial outcomes.…”

Section: What Is Known About Disclosure In Preclinical Ad?mentioning

confidence: 99%

“…The limited inclusiveness of biomarker research raises concerns about the validity of biomarker data in these populations. Data has shown that biomarker changes in AD can vary between Blacks and Whites, and similar biomarker profiles can be associated with divergent cognitive function 37 …”

Section: What Is Known About Disclosure In Preclinical Ad?mentioning

confidence: 99%

“…There is a pressing need for research in more diverse populations to make evidence about safety and prognosis more generalizable. The data used for current prognostic models largely come from non‐Hispanic White study participants, and may not be applicable to other racially and ethnically minoritized groups 37 . Similarly, safety outcomes after disclosure among general clinical populations may not be the same as the participants in biomarker research studies.…”

Section: How Can the Hd Framework Inform Research In Preclinical Ad?mentioning

confidence: 99%

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Moving beyond disclosure: Stages of care in preclinical Alzheimer's disease biomarker testing

Ketchum

Chin

Grill

et al. 2022

Alzheimer's & Dementia

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Alzheimer's disease (AD) begins with an asymptomatic “preclinical” phase, in which abnormal biomarkers indicate risk for developing cognitive impairment. Biomarker information is increasingly being disclosed in research settings, and is moving toward clinical settings with the development of cheaper and non‐invasive testing. Limited research has focused on the safety and psychological effects of disclosing biomarker results to cognitively unimpaired adults. However, less is known about how to ensure equitable access and robust counseling for decision‐making before testing, and how to effectively provide long‐term follow‐up and risk management after testing. Using the framework of Huntington's disease, which is based on extensive experience with disclosing and managing risk for a progressive neurodegenerative condition, this article proposes a conceptual model of pre‐disclosure, disclosure, and post‐disclosure phases for AD biomarker testing. Addressing research questions in each phase will facilitate the transition of biomarker testing into clinical practice.

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Section: What Is Known About Disclosure In Preclinical Ad?mentioning

confidence: 99%

Section: What Is Known About Disclosure In Preclinical Ad?mentioning

confidence: 99%

Section: How Can the Hd Framework Inform Research In Preclinical Ad?mentioning

confidence: 99%

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Moving beyond disclosure: Stages of care in preclinical Alzheimer's disease biomarker testing

Ketchum

Chin

Grill

et al. 2022

Alzheimer's & Dementia

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“…The limited inclusiveness of biomarker study samples raises concerns about the validity and reliability of biomarker data in underrepresented groups [ 19 ]. Data shows that biomarker changes in AD can vary between Black/African American and White populations, and similar biomarker profiles can be associated with divergent cognitive function [ 20, 21 ]. The current lack of reliable biomarker data for underrepresented groups limits the diagnostic, prognostic, and therapeutic validity of biomarkers for clinical use in these populations, and has the potential to further exacerbate health disparities [ 9 ].…”

Section: Introductionmentioning

confidence: 99%

What Influences the Willingness of Blacks and African Americans to Enroll in Preclinical Alzheimer’s Disease Biomarker Research? A Qualitative Vignette Analysis

Ketchum

Erickson

Chin

et al. 2022

JAD

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Background: Alzheimer’s disease (AD) begins with an asymptomatic “preclinical” phase, in which abnormal biomarkers indicate risk for developing cognitive impairment. Research is increasingly focused on validating biomarkers to improve reliable diagnosis and timely clinical treatment of AD. Most preclinical biomarker research lacks adequate representation of Black/African American and other racially and ethnically minoritized individuals, limiting the applicability of data to these groups. This may exacerbate existing disparities by hindering diagnosis and treatment among racially and ethnically minoritized individuals. Objective: Understand the factors influencing willingness of Blacks/African Americans to participate in AD biomarker research and identify opportunities to improve enrollment. Methods: We enrolled Blacks/African Americans (N = 145) between 46–85 years of age who had previously participated in AD research. Participants gave open-ended responses to a vignette describing a hypothetical biomarker research study. Using qualitative content analysis, we identified themes that motivated and discouraged enrollment in AD biomarker research. Results: Participant responses were categorized into several themes. Themes motivating participation included a desire to know their biomarker results and to support research. Major themes discouraging participation included concerns about potential negative psychological outcomes to learning one’s increased risk for AD, doubt about the usefulness of testing, and worry about the potential physical harms of testing. Conclusion: Understanding themes motivating and discouraging AD preclinical biomarker research participation may inform research material development, approach to community engagement, and/or trial design to increase enrollment of Blacks/African Americans.

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“…Furthermore, individual factors modify the relationship between tau accumulation and cognition, with younger age, female sex, higher educational attainment, and higher baseline cortical thickness all associated with increased resistance against the deleterious effect of pathology on cognitive performance (30). Some studies suggest that the relationship between tau, neurodegeneration, and cognition may also vary with race and ethnicity as proxies for social determinants of health (31), though much more work on diverse cohorts is needed to better understand these relationships. Finally, the development of biomarkers that measure common non-AD pathologies (e.g., vascular lesions, TDP43, and a-synuclein aggregates) will be critical for achieving a more adequate prognosis, as these processes are highly prevalent in patients with AD (32) and contribute significantly to neurodegeneration and cognitive decline.…”

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confidence: 99%

Tau Beats Amyloid in Predicting Brain Atrophy in Alzheimer Disease: Implications for Prognosis and Clinical Trials

2022

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Sever al biomarkers have emerged in the past few decades to quantify pathologic brain changes related to Alzheimer disease (AD). In particular, PET radiotracers that bind selectively to amyloid-b plaques and tau neurofibrillary tangles have advanced AD research and drug development by enabling the detection and quantification of the neuropathologic lesions that define AD in living people.Among amyloid-b PET tracers, 11 C-Pittsburgh compound B was the first to be developed, followed by 18 F-labeled tracers approved for clinical use (i.e., 18 F-florbetapir, 18 F-florbetaben, and 18

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Alzheimer's disease biomarkers in Black and non‐Hispanic White cohorts: A contextualized review of the evidence

Cited by 40 publications

References 112 publications

Moving beyond disclosure: Stages of care in preclinical Alzheimer's disease biomarker testing

Moving beyond disclosure: Stages of care in preclinical Alzheimer's disease biomarker testing

What Influences the Willingness of Blacks and African Americans to Enroll in Preclinical Alzheimer’s Disease Biomarker Research? A Qualitative Vignette Analysis

Tau Beats Amyloid in Predicting Brain Atrophy in Alzheimer Disease: Implications for Prognosis and Clinical Trials

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