Proteomics analysis of plasma from middle-aged adults identifies protein markers of dementia risk in later life.

TitleProteomics analysis of plasma from middle-aged adults identifies protein markers of dementia risk in later life.
Publication TypeJournal Article
Year of Publication2023
AuthorsWalker, KA, Chen, J, Shi, L, Yang, Y, Fornage, M, Zhou, L, Schlosser, P, Surapaneni, A, Grams, ME, Duggan, MR, Peng, Z, Gomez, GT, Tin, A, Hoogeveen, RC, Sullivan, KJ, Ganz, P, Lindbohm, JV, Kivimaki, M, Nevado-Holgado, AJ, Buckley, N, Gottesman, RF, Mosley, TH, Boerwinkle, E, Ballantyne, CM, Coresh, J
JournalSci Transl Med
Volume15
Issue705
Paginationeadf5681
Date Published2023 Jul 19
ISSN1946-6242
KeywordsAdult, Alzheimer Disease, Amyloid beta-Peptides, Biomarkers, Brain, Humans, Middle Aged, Proteomics, tau Proteins
Abstract

A diverse set of biological processes have been implicated in the pathophysiology of Alzheimer's disease (AD) and related dementias. However, there is limited understanding of the peripheral biological mechanisms relevant in the earliest phases of the disease. Here, we used a large-scale proteomics platform to examine the association of 4877 plasma proteins with 25-year dementia risk in 10,981 middle-aged adults. We found 32 dementia-associated plasma proteins that were involved in proteostasis, immunity, synaptic function, and extracellular matrix organization. We then replicated the association between 15 of these proteins and clinically relevant neurocognitive outcomes in two independent cohorts. We demonstrated that 12 of these 32 dementia-associated proteins were associated with cerebrospinal fluid (CSF) biomarkers of AD, neurodegeneration, or neuroinflammation. We found that eight of these candidate protein markers were abnormally expressed in human postmortem brain tissue from patients with AD, although some of the proteins that were most strongly associated with dementia risk, such as GDF15, were not detected in these brain tissue samples. Using network analyses, we found a protein signature for dementia risk that was characterized by dysregulation of specific immune and proteostasis/autophagy pathways in adults in midlife ~20 years before dementia onset, as well as abnormal coagulation and complement signaling ~10 years before dementia onset. Bidirectional two-sample Mendelian randomization genetically validated nine of our candidate proteins as markers of AD in midlife and inferred causality of SERPINA3 in AD pathogenesis. Last, we prioritized a set of candidate markers for AD and dementia risk prediction in midlife.

DOI10.1126/scitranslmed.adf5681
Alternate JournalSci Transl Med
PubMed ID37467317
PubMed Central IDPMC10665113
Grant ListU01 HL096812 / HL / NHLBI NIH HHS / United States
UL1 RR025005 / RR / NCRR NIH HHS / United States
U01 HL096917 / HL / NHLBI NIH HHS / United States
R01 HL059367 / HL / NHLBI NIH HHS / United States
Z99 AG999999 / ImNIH / Intramural NIH HHS / United States
R01 HL086694 / HL / NHLBI NIH HHS / United States
K24 HL155861 / HL / NHLBI NIH HHS / United States
HHSN268201700001I / HL / NHLBI NIH HHS / United States
U01 HL096814 / HL / NHLBI NIH HHS / United States
R01 HL070825 / HL / NHLBI NIH HHS / United States
R01 HL134320 / HL / NHLBI NIH HHS / United States
HHSN268201700003I / HL / NHLBI NIH HHS / United States
R01 AG056477 / AG / NIA NIH HHS / United States
R01 DK115534 / DK / NIDDK NIH HHS / United States
ZIA AG000348 / ImNIH / Intramural NIH HHS / United States
RF1 AG059421 / AG / NIA NIH HHS / United States
ZIA AG000349 / ImNIH / Intramural NIH HHS / United States
R024227/1 / MRC_ / Medical Research Council / United Kingdom
221854/Z/20/Z / WT_ / Wellcome Trust / United Kingdom
MRC S011676 / MRC_ / Medical Research Council / United Kingdom
MRC R024227/1 / MRC_ / Medical Research Council / United Kingdom
U01 HL096902 / HL / NHLBI NIH HHS / United States
MR/R024227/1 / MRC_ / Medical Research Council / United Kingdom
R01 AR073178 / AR / NIAMS NIH HHS / United States
HHSN268201700002C / HL / NHLBI NIH HHS / United States
RF1 AG062553 / AG / NIA NIH HHS / United States
U01 AG058589 / AG / NIA NIH HHS / United States
HHSN268201700004I / HL / NHLBI NIH HHS / United States
P30 AG066546 / AG / NIA NIH HHS / United States
MR/S011676/1 / MRC_ / Medical Research Council / United Kingdom
R01 DK108803 / DK / NIDDK NIH HHS / United States
U01 AG052409 / AG / NIA NIH HHS / United States
R01 DK124399 / DK / NIDDK NIH HHS / United States
HHSN268201700005C / HL / NHLBI NIH HHS / United States
HHSN268201700001C / HL / NHLBI NIH HHS / United States
HHSN268201700003C / HL / NHLBI NIH HHS / United States
U01 HL096899 / HL / NHLBI NIH HHS / United States
HHSN268201700004C / HL / NHLBI NIH HHS / United States
/ WT_ / Wellcome Trust / United Kingdom
HHSN268201700002I / HL / NHLBI NIH HHS / United States
HHSN268201700005I / HL / NHLBI NIH HHS / United States
R01 DK100446 / DK / NIDDK NIH HHS / United States
R01 HL087641 / HL / NHLBI NIH HHS / United States

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