CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death

An increased risk of cardiovascular death in Cytomegalovirus (CMV)-infected individuals remains unexplained, although it might partly result from the fact that CMV infection is closely associated with the accumulation of CD28(null) T-cells, in particular CD28(null) CD4 T-cells. These cells can direc...

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Autores principales: Pera, Alejandra, Caserta, Stefano, Albanese, Fabio, Blowers, Pinar, Morrow, George, Terrazzini, Nadia, Smith, Helen E, Rajkumar, Chakravarthi, Reus, Bernhard, Msonda, James R, Verboom, Murielle, Hallensleben, Michael, Blasczyk, Rainer, Davies, Kevin A, Kern, Florian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6134924/
https://www.ncbi.nlm.nih.gov/pubmed/30214635
http://dx.doi.org/10.7150/thno.27428
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author Pera, Alejandra
Caserta, Stefano
Albanese, Fabio
Blowers, Pinar
Morrow, George
Terrazzini, Nadia
Smith, Helen E
Rajkumar, Chakravarthi
Reus, Bernhard
Msonda, James R
Verboom, Murielle
Hallensleben, Michael
Blasczyk, Rainer
Davies, Kevin A
Kern, Florian
author_facet Pera, Alejandra
Caserta, Stefano
Albanese, Fabio
Blowers, Pinar
Morrow, George
Terrazzini, Nadia
Smith, Helen E
Rajkumar, Chakravarthi
Reus, Bernhard
Msonda, James R
Verboom, Murielle
Hallensleben, Michael
Blasczyk, Rainer
Davies, Kevin A
Kern, Florian
author_sort Pera, Alejandra
collection PubMed
description An increased risk of cardiovascular death in Cytomegalovirus (CMV)-infected individuals remains unexplained, although it might partly result from the fact that CMV infection is closely associated with the accumulation of CD28(null) T-cells, in particular CD28(null) CD4 T-cells. These cells can directly damage endothelium and precipitate cardiovascular events. However, the current paradigm holds that the accumulation of CD28(null) T-cells is a normal consequence of aging, whereas the link between these T-cell populations and CMV infection is explained by the increased prevalence of this infection in older people. Resolving whether CMV infection or aging triggers CD28(null) T-cell expansions is of critical importance because, unlike aging, CMV infection can be treated. Methods: We used multi-color flow-cytometry, antigen-specific activation assays, and HLA-typing to dissect the contributions of CMV infection and aging to the accumulation of CD28(null) CD4 and CD8 T-cells in CMV+ and CMV- individuals aged 19 to 94 years. Linear/logistic regression was used to test the effect of sex, age, CMV infection, and HLA-type on CD28(null) T-cell frequencies. Results: The median frequencies of CD28(null) CD4 T-cells and CD28(null) CD8 T-cells were >12-fold (p=0.000) but only approximately 2-fold higher (p=0.000), respectively, in CMV+ (n=136) compared with CMV- individuals (n=106). The effect of CMV infection on these T-cell subsets was confirmed by linear regression. Unexpectedly, aging contributed only marginally to an increase in CD28(null) T-cell frequencies, and only in CMV+ individuals. Interestingly, the presence of HLA-DRB1*0301 led to an approximately 9-fold reduction of the risk of having CD28(null) CD4 T-cell expansions (OR=0.108, p=0.003). Over 75% of CMV-reactive CD4 T-cells were CD28(null). Conclusion: CMV infection and HLA type are major risk factors for CD28(null) CD4 T-cell-associated cardiovascular pathology. Increased numbers of CD28(null) CD8 T-cells are also associated with CMV infection, but to a lesser extent. Aging, however, makes only a negligible contribution to the expansion of these T-cell subsets, and only in the presence of CMV infection. Our results open up new avenues for risk assessment, prevention, and treatment.
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spelling pubmed-61349242018-09-13 CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death Pera, Alejandra Caserta, Stefano Albanese, Fabio Blowers, Pinar Morrow, George Terrazzini, Nadia Smith, Helen E Rajkumar, Chakravarthi Reus, Bernhard Msonda, James R Verboom, Murielle Hallensleben, Michael Blasczyk, Rainer Davies, Kevin A Kern, Florian Theranostics Research Paper An increased risk of cardiovascular death in Cytomegalovirus (CMV)-infected individuals remains unexplained, although it might partly result from the fact that CMV infection is closely associated with the accumulation of CD28(null) T-cells, in particular CD28(null) CD4 T-cells. These cells can directly damage endothelium and precipitate cardiovascular events. However, the current paradigm holds that the accumulation of CD28(null) T-cells is a normal consequence of aging, whereas the link between these T-cell populations and CMV infection is explained by the increased prevalence of this infection in older people. Resolving whether CMV infection or aging triggers CD28(null) T-cell expansions is of critical importance because, unlike aging, CMV infection can be treated. Methods: We used multi-color flow-cytometry, antigen-specific activation assays, and HLA-typing to dissect the contributions of CMV infection and aging to the accumulation of CD28(null) CD4 and CD8 T-cells in CMV+ and CMV- individuals aged 19 to 94 years. Linear/logistic regression was used to test the effect of sex, age, CMV infection, and HLA-type on CD28(null) T-cell frequencies. Results: The median frequencies of CD28(null) CD4 T-cells and CD28(null) CD8 T-cells were >12-fold (p=0.000) but only approximately 2-fold higher (p=0.000), respectively, in CMV+ (n=136) compared with CMV- individuals (n=106). The effect of CMV infection on these T-cell subsets was confirmed by linear regression. Unexpectedly, aging contributed only marginally to an increase in CD28(null) T-cell frequencies, and only in CMV+ individuals. Interestingly, the presence of HLA-DRB1*0301 led to an approximately 9-fold reduction of the risk of having CD28(null) CD4 T-cell expansions (OR=0.108, p=0.003). Over 75% of CMV-reactive CD4 T-cells were CD28(null). Conclusion: CMV infection and HLA type are major risk factors for CD28(null) CD4 T-cell-associated cardiovascular pathology. Increased numbers of CD28(null) CD8 T-cells are also associated with CMV infection, but to a lesser extent. Aging, however, makes only a negligible contribution to the expansion of these T-cell subsets, and only in the presence of CMV infection. Our results open up new avenues for risk assessment, prevention, and treatment. Ivyspring International Publisher 2018-08-07 /pmc/articles/PMC6134924/ /pubmed/30214635 http://dx.doi.org/10.7150/thno.27428 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Pera, Alejandra
Caserta, Stefano
Albanese, Fabio
Blowers, Pinar
Morrow, George
Terrazzini, Nadia
Smith, Helen E
Rajkumar, Chakravarthi
Reus, Bernhard
Msonda, James R
Verboom, Murielle
Hallensleben, Michael
Blasczyk, Rainer
Davies, Kevin A
Kern, Florian
CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title_full CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title_fullStr CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title_full_unstemmed CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title_short CD28(null) pro-atherogenic CD4 T-cells explain the link between CMV infection and an increased risk of cardiovascular death
title_sort cd28(null) pro-atherogenic cd4 t-cells explain the link between cmv infection and an increased risk of cardiovascular death
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6134924/
https://www.ncbi.nlm.nih.gov/pubmed/30214635
http://dx.doi.org/10.7150/thno.27428
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