WMH Contributions to Cognitive Impairment: Rationale and Design of the Diverse VCID Study

doi:10.1161/STROKEAHA.124.045903

WMH Contributions to Cognitive Impairment: Rationale and Design of the Diverse VCID Study

Research output: Contribution to journal › Review article › peer-review

5 Scopus citations

Abstract

As awareness of dementia increases, more individuals with minor cognitive complaints are requesting clinical assessment. Neuroimaging studies frequently identify incidental white matter hyperintensities, raising patient concerns about their brain health and future risk for dementia. Moreover, current US demographics indicate that ≈50% of these individuals will be from diverse backgrounds by 2060. Racial and ethnic minority populations bear a disproportionate burden of vascular risk factors magnifying dementia risk. Despite established associations between white matter hyperintensities and cognitive impairment, including dementia, no study has comprehensively and prospectively examined the impact of individual and combined magnetic resonance imaging measures of white matter injury, their risk factors, and comorbidities on cognitive performance among a diverse, nondemented, stroke-free population with cognitive complaints over an extended period of observation. The Diverse VCID (Diverse Vascular Cognitive Impairment and Dementia) study is designed to fill this knowledge gap through 3 assessments of clinical, behavioral, and risk factors; neurocognitive and magnetic resonance imaging measures; fluid biomarkers of Alzheimer disease, vascular inflammation, angiogenesis, and endothelial dysfunction; and measures of genetic risk collected prospectively over a minimum of 3 years in a cohort of 2250 individuals evenly distributed among Americans of Black/African, Latino/Hispanic, and non-Hispanic White backgrounds. The goal of this study is to investigate the basic mechanisms of small vessel cerebrovascular injury, emphasizing clinically relevant assessment tools and developing a risk score that will accurately identify at-risk individuals for possible treatment or clinical therapeutic trials, particularly individuals of diverse backgrounds where vascular risk factors and disease are more prevalent.

Original language	English
Pages (from-to)	758-776
Number of pages	19
Journal	Stroke
Volume	56
Issue number	3
DOIs	https://doi.org/10.1161/STROKEAHA.124.045903
State	Published - Mar 1 2025

Bibliographical note

Publisher Copyright:
© 2024 American Heart Association, Inc.

Funding

Diverse VCID study (Diverse Vascular Cognitive Impairment and Dementia) is jointly supported by the National Institute of Neurological Disorders and Stroke and the National Institute on Aging under award U19NS120384. Dr DeCarli is supported in part by National Institutes of Health (NIH) grants P30 AG072972, U19NS120384, R01 AG075758, RF1 AG077639, and RF1 NS130659. He also serves as a consultant to Norvo Nordisk and Eisai Pharmaceuticals. Dr Rajan is supported in part by NIH grants R01 AG058679, R01 AG 065359, U19 NS 120384, and R01 AG 073627. Dr Jin is supported in part by NIH grants U19 NS120384, P30 AG072972, RF1 AG071665, RF1 AG052132, RF1 AG056519, and P01 AG025532. Dr Johnson is supported in part by NIH grants P30 AG072972 and U19NS120384 as well as CA Department of Public Health 18-10922, 22-10901, and 22-2948. Dr Harvey is supported in part by NIH grants P30AG072972, U19AG024904, and U19NS120384 and is consultant to NervGen. Dr Hinman is supported in part by NIH grants UF1NS100608, UF1NS100614, U19 NS120384, and U19NS115388. He is also employed by US Department of Veterans Affairs, has stock holdings in Sage Cerebrovascular Diagnostics, serves as President for Sage Cerebrovascular Diagnostics, and has a patent pending for Serologic assay for silent brain ischemia licensed to Sage Cerebrovascular Diagnostics. Dr Fornage is supported in part by NIH grants U19NS120384, R01AG075758, and UF1NS125513.

Funders	Funder number
Institute of Neurological Disorders and Stroke National Advisory Neurological Disorders and Stroke Council
National Institutes of Health (NIH)	R01 AG058679, RF1 AG052132, R01 AG 073627, RF1 NS130659, RF1 AG056519, R01 AG 065359, P30 AG072972, RF1 AG077639, R01 AG075758, P01 AG025532, RF1 AG071665
National Institutes of Health (NIH)
California Department of Public Health	P30AG072972, 22-2948, U19NS115388, UF1NS100608, R01AG075758, UF1NS100614, 22-10901, UF1NS125513, 18-10922, U19AG024904
California Department of Public Health
National Institute on Aging	U19NS120384
National Institute on Aging

Keywords

Alzheimer disease
cognitive dysfunction
dementia, vascular
neuroimaging
stroke
white matter

ASJC Scopus subject areas

Clinical Neurology
Cardiology and Cardiovascular Medicine
Advanced and Specialized Nursing

Access to Document

10.1161/STROKEAHA.124.045903

Cite this

@article{2687aa9048b24fadbbc5379e9beaee98,

title = "WMH Contributions to Cognitive Impairment: Rationale and Design of the Diverse VCID Study",

abstract = "As awareness of dementia increases, more individuals with minor cognitive complaints are requesting clinical assessment. Neuroimaging studies frequently identify incidental white matter hyperintensities, raising patient concerns about their brain health and future risk for dementia. Moreover, current US demographics indicate that ≈50\% of these individuals will be from diverse backgrounds by 2060. Racial and ethnic minority populations bear a disproportionate burden of vascular risk factors magnifying dementia risk. Despite established associations between white matter hyperintensities and cognitive impairment, including dementia, no study has comprehensively and prospectively examined the impact of individual and combined magnetic resonance imaging measures of white matter injury, their risk factors, and comorbidities on cognitive performance among a diverse, nondemented, stroke-free population with cognitive complaints over an extended period of observation. The Diverse VCID (Diverse Vascular Cognitive Impairment and Dementia) study is designed to fill this knowledge gap through 3 assessments of clinical, behavioral, and risk factors; neurocognitive and magnetic resonance imaging measures; fluid biomarkers of Alzheimer disease, vascular inflammation, angiogenesis, and endothelial dysfunction; and measures of genetic risk collected prospectively over a minimum of 3 years in a cohort of 2250 individuals evenly distributed among Americans of Black/African, Latino/Hispanic, and non-Hispanic White backgrounds. The goal of this study is to investigate the basic mechanisms of small vessel cerebrovascular injury, emphasizing clinically relevant assessment tools and developing a risk score that will accurately identify at-risk individuals for possible treatment or clinical therapeutic trials, particularly individuals of diverse backgrounds where vascular risk factors and disease are more prevalent.",

keywords = "Alzheimer disease, cognitive dysfunction, dementia, vascular, neuroimaging, stroke, white matter",

author = "Charles DeCarli and Rajan, \{Kumar B.\} and Jin, \{Lee Way\} and Jason Hinman and Johnson, \{David K.\} and Danielle Harvey and Myriam Fornage and Alexa Beiser and Hector Gonzalez and Walter Kukull and Lisa Barnes and Fanny Elahi and Raina Croff and Joel Kramer and Johannes Weickenmeier and Dana Tudorascu and Marilyn Albert and Suzanne Craft and Gregory Jicha and Wolk, \{David A.\} and Henry Paulson and James Brewer and Sanjay Asthana and Sudha Seshadri and Adam Brickman and Chui, \{Helena Chang\} and Amy Nelson and Sean Savitz and Andrew Saykin and David Geldmacher and Arjun Masurkar and Tatjana Rundek and Pauline Maillard and Alex Knaack",

note = "Publisher Copyright: {\textcopyright} 2024 American Heart Association, Inc.",

year = "2025",

month = mar,

day = "1",

doi = "10.1161/STROKEAHA.124.045903",

language = "English",

volume = "56",

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AU - DeCarli, Charles

AU - Rajan, Kumar B.

AU - Jin, Lee Way

AU - Hinman, Jason

AU - Johnson, David K.

AU - Harvey, Danielle

AU - Fornage, Myriam

AU - Beiser, Alexa

AU - Gonzalez, Hector

AU - Kukull, Walter

AU - Barnes, Lisa

AU - Elahi, Fanny

AU - Croff, Raina

AU - Kramer, Joel

AU - Weickenmeier, Johannes

AU - Tudorascu, Dana

AU - Albert, Marilyn

AU - Craft, Suzanne

AU - Jicha, Gregory

AU - Wolk, David A.

AU - Paulson, Henry

AU - Brewer, James

AU - Asthana, Sanjay

AU - Seshadri, Sudha

AU - Brickman, Adam

AU - Chui, Helena Chang

AU - Nelson, Amy

AU - Savitz, Sean

AU - Saykin, Andrew

AU - Geldmacher, David

AU - Masurkar, Arjun

AU - Rundek, Tatjana

AU - Maillard, Pauline

AU - Knaack, Alex

PY - 2025/3/1

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N2 - As awareness of dementia increases, more individuals with minor cognitive complaints are requesting clinical assessment. Neuroimaging studies frequently identify incidental white matter hyperintensities, raising patient concerns about their brain health and future risk for dementia. Moreover, current US demographics indicate that ≈50% of these individuals will be from diverse backgrounds by 2060. Racial and ethnic minority populations bear a disproportionate burden of vascular risk factors magnifying dementia risk. Despite established associations between white matter hyperintensities and cognitive impairment, including dementia, no study has comprehensively and prospectively examined the impact of individual and combined magnetic resonance imaging measures of white matter injury, their risk factors, and comorbidities on cognitive performance among a diverse, nondemented, stroke-free population with cognitive complaints over an extended period of observation. The Diverse VCID (Diverse Vascular Cognitive Impairment and Dementia) study is designed to fill this knowledge gap through 3 assessments of clinical, behavioral, and risk factors; neurocognitive and magnetic resonance imaging measures; fluid biomarkers of Alzheimer disease, vascular inflammation, angiogenesis, and endothelial dysfunction; and measures of genetic risk collected prospectively over a minimum of 3 years in a cohort of 2250 individuals evenly distributed among Americans of Black/African, Latino/Hispanic, and non-Hispanic White backgrounds. The goal of this study is to investigate the basic mechanisms of small vessel cerebrovascular injury, emphasizing clinically relevant assessment tools and developing a risk score that will accurately identify at-risk individuals for possible treatment or clinical therapeutic trials, particularly individuals of diverse backgrounds where vascular risk factors and disease are more prevalent.

AB - As awareness of dementia increases, more individuals with minor cognitive complaints are requesting clinical assessment. Neuroimaging studies frequently identify incidental white matter hyperintensities, raising patient concerns about their brain health and future risk for dementia. Moreover, current US demographics indicate that ≈50% of these individuals will be from diverse backgrounds by 2060. Racial and ethnic minority populations bear a disproportionate burden of vascular risk factors magnifying dementia risk. Despite established associations between white matter hyperintensities and cognitive impairment, including dementia, no study has comprehensively and prospectively examined the impact of individual and combined magnetic resonance imaging measures of white matter injury, their risk factors, and comorbidities on cognitive performance among a diverse, nondemented, stroke-free population with cognitive complaints over an extended period of observation. The Diverse VCID (Diverse Vascular Cognitive Impairment and Dementia) study is designed to fill this knowledge gap through 3 assessments of clinical, behavioral, and risk factors; neurocognitive and magnetic resonance imaging measures; fluid biomarkers of Alzheimer disease, vascular inflammation, angiogenesis, and endothelial dysfunction; and measures of genetic risk collected prospectively over a minimum of 3 years in a cohort of 2250 individuals evenly distributed among Americans of Black/African, Latino/Hispanic, and non-Hispanic White backgrounds. The goal of this study is to investigate the basic mechanisms of small vessel cerebrovascular injury, emphasizing clinically relevant assessment tools and developing a risk score that will accurately identify at-risk individuals for possible treatment or clinical therapeutic trials, particularly individuals of diverse backgrounds where vascular risk factors and disease are more prevalent.

KW - Alzheimer disease

KW - cognitive dysfunction

KW - dementia, vascular

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KW - stroke

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WMH Contributions to Cognitive Impairment: Rationale and Design of the Diverse VCID Study

Abstract

Bibliographical note

Funding

Keywords

ASJC Scopus subject areas

Access to Document

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