Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.

Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.

Chronic activation of the complement system and induced inflammation are associated with neuropathology in Alzheimer's disease (AD). Recent large genome wide association studies (GWAS) have identified single nucleotide polymorphisms (SNPs) in the C3b/C4b receptor (CR1 or CD35) that are associat...

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Main Authors: Maria I Fonseca, Shuhui Chu, Aimee L Pierce, William D Brubaker, Richard E Hauhart, Diego Mastroeni, Elizabeth V Clarke, Joseph Rogers, John P Atkinson, Andrea J Tenner
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4767815?pdf=render
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spelling doaj-e80b68870340438f96ecae3c7cc77d032020-11-25T00:59:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01112e014979210.1371/journal.pone.0149792Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.Maria I FonsecaShuhui ChuAimee L PierceWilliam D BrubakerRichard E HauhartDiego MastroeniElizabeth V ClarkeJoseph RogersJohn P AtkinsonAndrea J TennerChronic activation of the complement system and induced inflammation are associated with neuropathology in Alzheimer's disease (AD). Recent large genome wide association studies (GWAS) have identified single nucleotide polymorphisms (SNPs) in the C3b/C4b receptor (CR1 or CD35) that are associated with late onset AD. Here, anti-CR1 antibodies (Abs) directed against different epitopes of the receptor, were used to localize CR1 in brain, and relative binding affinities of the CR1 ligands, C1q and C3b, were assessed by ELISA. Most Abs tested stained red blood cells in blood vessels but showed no staining in brain parenchyma. However, two monoclonal anti-CR1 Abs labeled astrocytes in all of the cases tested, and this reactivity was preabsorbed by purified recombinant human CR1. Human brain-derived astrocyte cultures were also reactive with both mAbs. The amount of astrocyte staining varied among the samples, but no consistent difference was conferred by diagnosis or the GWAS-identified SNPs rs4844609 or rs6656401. Plasma levels of soluble CR1 did not correlate with diagnosis but a slight increase was observed with rs4844609 and rs6656401 SNP. There was also a modest but statistically significant increase in relative binding activity of C1q to CR1 with the rs4844609 SNP compared to CR1 without the SNP, and of C3b to CR1 in the CR1 genotypes containing the rs6656401 SNP (also associated with the larger isoform of CR1) regardless of clinical diagnosis. These results suggest that it is unlikely that astrocyte CR1 expression levels or C1q or C3b binding activity are the cause of the GWAS identified association of CR1 variants with AD. Further careful functional studies are needed to determine if the variant-dictated number of CR1 expressed on red blood cells contributes to the role of this receptor in the progression of AD, or if another mechanism is involved.http://europepmc.org/articles/PMC4767815?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Maria I Fonseca
Shuhui Chu
Aimee L Pierce
William D Brubaker
Richard E Hauhart
Diego Mastroeni
Elizabeth V Clarke
Joseph Rogers
John P Atkinson
Andrea J Tenner
spellingShingle Maria I Fonseca
Shuhui Chu
Aimee L Pierce
William D Brubaker
Richard E Hauhart
Diego Mastroeni
Elizabeth V Clarke
Joseph Rogers
John P Atkinson
Andrea J Tenner
Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
PLoS ONE
author_facet Maria I Fonseca
Shuhui Chu
Aimee L Pierce
William D Brubaker
Richard E Hauhart
Diego Mastroeni
Elizabeth V Clarke
Joseph Rogers
John P Atkinson
Andrea J Tenner
author_sort Maria I Fonseca
title Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
title_short Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
title_full Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
title_fullStr Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
title_full_unstemmed Analysis of the Putative Role of CR1 in Alzheimer's Disease: Genetic Association, Expression and Function.
title_sort analysis of the putative role of cr1 in alzheimer's disease: genetic association, expression and function.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2016-01-01
description Chronic activation of the complement system and induced inflammation are associated with neuropathology in Alzheimer's disease (AD). Recent large genome wide association studies (GWAS) have identified single nucleotide polymorphisms (SNPs) in the C3b/C4b receptor (CR1 or CD35) that are associated with late onset AD. Here, anti-CR1 antibodies (Abs) directed against different epitopes of the receptor, were used to localize CR1 in brain, and relative binding affinities of the CR1 ligands, C1q and C3b, were assessed by ELISA. Most Abs tested stained red blood cells in blood vessels but showed no staining in brain parenchyma. However, two monoclonal anti-CR1 Abs labeled astrocytes in all of the cases tested, and this reactivity was preabsorbed by purified recombinant human CR1. Human brain-derived astrocyte cultures were also reactive with both mAbs. The amount of astrocyte staining varied among the samples, but no consistent difference was conferred by diagnosis or the GWAS-identified SNPs rs4844609 or rs6656401. Plasma levels of soluble CR1 did not correlate with diagnosis but a slight increase was observed with rs4844609 and rs6656401 SNP. There was also a modest but statistically significant increase in relative binding activity of C1q to CR1 with the rs4844609 SNP compared to CR1 without the SNP, and of C3b to CR1 in the CR1 genotypes containing the rs6656401 SNP (also associated with the larger isoform of CR1) regardless of clinical diagnosis. These results suggest that it is unlikely that astrocyte CR1 expression levels or C1q or C3b binding activity are the cause of the GWAS identified association of CR1 variants with AD. Further careful functional studies are needed to determine if the variant-dictated number of CR1 expressed on red blood cells contributes to the role of this receptor in the progression of AD, or if another mechanism is involved.
url http://europepmc.org/articles/PMC4767815?pdf=render
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