Inflammatory plasma biomarkers in subjects with preclinical Alzheimer's disease.
Eotaxin-1
GFAP
MCP-1
Neuroinflammation
Preclinical Alzheimer’s disease
YKL-40
Journal
Alzheimer's research & therapy
ISSN: 1758-9193
Titre abrégé: Alzheimers Res Ther
Pays: England
ID NLM: 101511643
Informations de publication
Date de publication:
03 08 2022
03 08 2022
Historique:
received:
23
11
2021
accepted:
21
07
2022
entrez:
3
8
2022
pubmed:
4
8
2022
medline:
6
8
2022
Statut:
epublish
Résumé
This study investigated plasma biomarkers for neuroinflammation associated with Alzheimer's disease (AD) in subjects with preclinical AD compared to healthy elderly. How these biomarkers behave in patients with AD, compared to healthy elderly is well known, but determining these in subjects with preclinical AD is not and will add information related to the onset of AD. When found to be different in preclinical AD, these inflammatory biomarkers may be used to select preclinical AD subjects who are most likely to develop AD, to participate in clinical trials with new disease-modifying drugs. Healthy elderly (n= 50; age 71.9; MMSE >24) and subjects with preclinical AD (n=50; age 73.4; MMSE >24) defined by CSF Aβ1-42 levels < 1000 pg/mL were included. Four neuroinflammatory biomarkers were determined in plasma, GFAP, YKL-40, MCP-1, and eotaxin-1. Differences in biomarker outcomes were compared using ANCOVA. Subject characteristics age, gender, and APOE ε4 status were reported per group and were covariates in the ANCOVA. Least square means were calculated for all 4 inflammatory biomarkers using both the Aβ+/Aβ- cutoff and Ptau/Aβ1-42 ratio. The mean (standard deviation, SD) age of the subjects (n=100) was 72.6 (4.6) years old with 62 male and 38 female subjects. Mean (SD) overall MMSE score was 28.7 (0.49) and 32 subjects were APOE ε4 carriers. The number of subjects in the different APOE ε4 status categories differed significantly between the Aβ+ and Aβ- groups. Plasma GFAP concentration was significantly higher in the Aβ+ group compared to the Aβ- group with significant covariates age and sex, variables that also correlated significantly with GFAP. GFAP was significantly higher in subjects with preclinical AD compared to healthy elderly which agrees with previous studies. When defining preclinical AD based on the Ptau181/Aβ1-42 ratio, YKL-40 was also significantly different between groups. This could indicate that GFAP and YKL-40 are more sensitive markers of the inflammatory process in response to the Aβ misfolding and aggregation that is ongoing as indicated by the lowered Aβ1-42 levels in the CSF. Characterizing subjects with preclinical AD using neuroinflammatory biomarkers is important for subject selection in new disease-modifying clinical trials. ISRCTN.org identifier: ISRCTN79036545 (retrospectively registered).
Sections du résumé
BACKGROUND
This study investigated plasma biomarkers for neuroinflammation associated with Alzheimer's disease (AD) in subjects with preclinical AD compared to healthy elderly. How these biomarkers behave in patients with AD, compared to healthy elderly is well known, but determining these in subjects with preclinical AD is not and will add information related to the onset of AD. When found to be different in preclinical AD, these inflammatory biomarkers may be used to select preclinical AD subjects who are most likely to develop AD, to participate in clinical trials with new disease-modifying drugs.
METHODS
Healthy elderly (n= 50; age 71.9; MMSE >24) and subjects with preclinical AD (n=50; age 73.4; MMSE >24) defined by CSF Aβ1-42 levels < 1000 pg/mL were included. Four neuroinflammatory biomarkers were determined in plasma, GFAP, YKL-40, MCP-1, and eotaxin-1. Differences in biomarker outcomes were compared using ANCOVA. Subject characteristics age, gender, and APOE ε4 status were reported per group and were covariates in the ANCOVA. Least square means were calculated for all 4 inflammatory biomarkers using both the Aβ+/Aβ- cutoff and Ptau/Aβ1-42 ratio.
RESULTS
The mean (standard deviation, SD) age of the subjects (n=100) was 72.6 (4.6) years old with 62 male and 38 female subjects. Mean (SD) overall MMSE score was 28.7 (0.49) and 32 subjects were APOE ε4 carriers. The number of subjects in the different APOE ε4 status categories differed significantly between the Aβ+ and Aβ- groups. Plasma GFAP concentration was significantly higher in the Aβ+ group compared to the Aβ- group with significant covariates age and sex, variables that also correlated significantly with GFAP.
CONCLUSION
GFAP was significantly higher in subjects with preclinical AD compared to healthy elderly which agrees with previous studies. When defining preclinical AD based on the Ptau181/Aβ1-42 ratio, YKL-40 was also significantly different between groups. This could indicate that GFAP and YKL-40 are more sensitive markers of the inflammatory process in response to the Aβ misfolding and aggregation that is ongoing as indicated by the lowered Aβ1-42 levels in the CSF. Characterizing subjects with preclinical AD using neuroinflammatory biomarkers is important for subject selection in new disease-modifying clinical trials.
TRIAL REGISTRATION
ISRCTN.org identifier: ISRCTN79036545 (retrospectively registered).
Identifiants
pubmed: 35922871
doi: 10.1186/s13195-022-01051-2
pii: 10.1186/s13195-022-01051-2
pmc: PMC9347121
doi:
Substances chimiques
Amyloid beta-Peptides
0
Apolipoprotein E4
0
Biomarkers
0
Chitinase-3-Like Protein 1
0
Peptide Fragments
0
tau Proteins
0
Banques de données
ISRCTN
['ISRCTN79036545']
Types de publication
Clinical Trial
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
106Informations de copyright
© 2022. The Author(s).
Références
Lancet Neurol. 2016 Jun;15(7):673-684
pubmed: 27068280
Alzheimers Res Ther. 2015 Dec 24;7:74
pubmed: 26698298
Alzheimers Dement (Amst). 2016 Jun 22;3:91-7
pubmed: 27453930
Lancet Neurol. 2015 Apr;14(4):388-405
pubmed: 25792098
Nat Immunol. 2001 Feb;2(2):95-101
pubmed: 11175800
Adv Med Sci. 2015 Mar;60(1):76-82
pubmed: 25579841
J Alzheimers Dis. 2019;67(2):481-488
pubmed: 30594925
Neurol Sci. 2020 Dec;41(12):3609-3615
pubmed: 32458252
Sci Rep. 2019 Dec 13;9(1):19024
pubmed: 31836810
Psychiatry Clin Neurosci. 1998 Dec;52(6):593-9
pubmed: 9895207
J Biomed Sci. 2020 Jan 6;27(1):18
pubmed: 31906949
Alzheimers Res Ther. 2021 Jul 17;13(1):132
pubmed: 34274005
J Appl Lab Med. 2020 Jan 1;5(1):194-208
pubmed: 31843944
Alzheimers Dement (Amst). 2021 May 01;13(1):e12182
pubmed: 33969174
Neurology. 2009 Dec 1;73(22):1914-22
pubmed: 19949037
Alzheimers Dement (Amst). 2021 May 18;13(1):e12190
pubmed: 34027020
Neurobiol Aging. 2020 Dec;96:22-32
pubmed: 32920471
Brain. 2021 Dec 16;144(11):3505-3516
pubmed: 34259835
Transl Psychiatry. 2021 Jan 11;11(1):27
pubmed: 33431793
Alzheimers Dement. 2019 Jun;15(6):776-787
pubmed: 31047856
Mult Scler. 2020 Feb;26(2):210-219
pubmed: 30570436
JAMA Intern Med. 2021 Oct 1;181(10):1276-1278
pubmed: 34254984
Mol Psychiatry. 2021 Jan;26(1):296-308
pubmed: 32251378
Front Aging Neurosci. 2020 Sep 02;12:272
pubmed: 32982716
Scand J Infect Dis. 2002;34(5):323-6
pubmed: 12069012
J Intern Med. 2018 Dec;284(6):643-663
pubmed: 30051512
J Alzheimers Dis. 2009;17(3):541-51
pubmed: 19433893
J Neuroinflammation. 2019 Jul 12;16(1):145
pubmed: 31299989
Expert Rev Proteomics. 2017 Apr;14(4):285-299
pubmed: 28281838
JAMA. 2015 May 19;313(19):1924-38
pubmed: 25988462
J Crit Care. 2019 Aug;52:172-179
pubmed: 31078998