Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation

BACKGROUND: Epicardial adipose tissue (EAT) directly overlies the myocardium, with changes in its morphology and volume associated with myriad cardiovascular and metabolic diseases. However, EAT’s immune structure and cellular characterization remain incompletely described. We aimed to define the im...

Descripción completa

Detalles Bibliográficos
Autores principales: Vyas, Vishal, Blythe, Hazel, Wood, Elizabeth G., Sandhar, Balraj, Sarker, Shah-Jalal, Balmforth, Damian, Ambekar, Shirish G., Yap, John, Edmondson, Stephen J., Di Salvo, Carmelo, Wong, Kit, Roberts, Neil, Uppal, Rakesh, Adams, Ben, Shipolini, Alex, Oo, Aung Y., Lawrence, David, Kolvekar, Shyam, Lall, Kulvinder S., Finlay, Malcolm C., Longhi, M. Paula
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2021
Materias:
Clinical Medicine
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8409986/
https://www.ncbi.nlm.nih.gov/pubmed/34283808
http://dx.doi.org/10.1172/jci.insight.145495
_version_ 1783747072115081216
author Vyas, Vishal
Blythe, Hazel
Wood, Elizabeth G.
Sandhar, Balraj
Sarker, Shah-Jalal
Balmforth, Damian
Ambekar, Shirish G.
Yap, John
Edmondson, Stephen J.
Di Salvo, Carmelo
Wong, Kit
Roberts, Neil
Uppal, Rakesh
Adams, Ben
Shipolini, Alex
Oo, Aung Y.
Lawrence, David
Kolvekar, Shyam
Lall, Kulvinder S.
Finlay, Malcolm C.
Longhi, M. Paula
author_facet Vyas, Vishal
Blythe, Hazel
Wood, Elizabeth G.
Sandhar, Balraj
Sarker, Shah-Jalal
Balmforth, Damian
Ambekar, Shirish G.
Yap, John
Edmondson, Stephen J.
Di Salvo, Carmelo
Wong, Kit
Roberts, Neil
Uppal, Rakesh
Adams, Ben
Shipolini, Alex
Oo, Aung Y.
Lawrence, David
Kolvekar, Shyam
Lall, Kulvinder S.
Finlay, Malcolm C.
Longhi, M. Paula
author_sort Vyas, Vishal
collection PubMed
description BACKGROUND: Epicardial adipose tissue (EAT) directly overlies the myocardium, with changes in its morphology and volume associated with myriad cardiovascular and metabolic diseases. However, EAT’s immune structure and cellular characterization remain incompletely described. We aimed to define the immune phenotype of EAT in humans and compare such profiles across lean, obese, and diabetic patients. METHODS: We recruited 152 patients undergoing open-chest coronary artery bypass grafting (CABG), valve repair/replacement (VR) surgery, or combined CABG/VR. Patients’ clinical and biochemical data and EAT, subcutaneous adipose tissue (SAT), and preoperative blood samples were collected. Immune cell profiling was evaluated by flow cytometry and complemented by gene expression studies of immune mediators. Bulk RNA-Seq was performed in EAT across metabolic profiles to assess whole-transcriptome changes observed in lean, obese, and diabetic groups. RESULTS: Flow cytometry analysis demonstrated EAT was highly enriched in adaptive immune (T and B) cells. Although overweight/obese and diabetic patients had similar EAT cellular profiles to lean control patients, the EAT exhibited significantly (P ≤ 0.01) raised expression of immune mediators, including IL-1, IL-6, TNF-α, and IFN-γ. These changes were not observed in SAT or blood. Neither underlying coronary artery disease nor the presence of hypertension significantly altered the immune profiles observed. Bulk RNA-Seq demonstrated significant alterations in metabolic and inflammatory pathways in the EAT of overweight/obese patients compared with lean controls. CONCLUSION: Adaptive immune cells are the predominant immune cell constituent in human EAT and SAT. The presence of underlying cardiometabolic conditions, specifically obesity and diabetes, rather than cardiac disease phenotype appears to alter the inflammatory profile of EAT. Obese states markedly alter EAT metabolic and inflammatory signaling genes, underlining the impact of obesity on the EAT transcriptome profile. FUNDING: Barts Charity MGU0413, Abbott, Medical Research Council MR/T008059/1, and British Heart Foundation FS/13/49/30421 and PG/16/79/32419.
format Online
Article
Text
id pubmed-8409986
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher American Society for Clinical Investigation
record_format MEDLINE/PubMed
spelling pubmed-84099862021-09-07 Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation Vyas, Vishal Blythe, Hazel Wood, Elizabeth G. Sandhar, Balraj Sarker, Shah-Jalal Balmforth, Damian Ambekar, Shirish G. Yap, John Edmondson, Stephen J. Di Salvo, Carmelo Wong, Kit Roberts, Neil Uppal, Rakesh Adams, Ben Shipolini, Alex Oo, Aung Y. Lawrence, David Kolvekar, Shyam Lall, Kulvinder S. Finlay, Malcolm C. Longhi, M. Paula JCI Insight Clinical Medicine BACKGROUND: Epicardial adipose tissue (EAT) directly overlies the myocardium, with changes in its morphology and volume associated with myriad cardiovascular and metabolic diseases. However, EAT’s immune structure and cellular characterization remain incompletely described. We aimed to define the immune phenotype of EAT in humans and compare such profiles across lean, obese, and diabetic patients. METHODS: We recruited 152 patients undergoing open-chest coronary artery bypass grafting (CABG), valve repair/replacement (VR) surgery, or combined CABG/VR. Patients’ clinical and biochemical data and EAT, subcutaneous adipose tissue (SAT), and preoperative blood samples were collected. Immune cell profiling was evaluated by flow cytometry and complemented by gene expression studies of immune mediators. Bulk RNA-Seq was performed in EAT across metabolic profiles to assess whole-transcriptome changes observed in lean, obese, and diabetic groups. RESULTS: Flow cytometry analysis demonstrated EAT was highly enriched in adaptive immune (T and B) cells. Although overweight/obese and diabetic patients had similar EAT cellular profiles to lean control patients, the EAT exhibited significantly (P ≤ 0.01) raised expression of immune mediators, including IL-1, IL-6, TNF-α, and IFN-γ. These changes were not observed in SAT or blood. Neither underlying coronary artery disease nor the presence of hypertension significantly altered the immune profiles observed. Bulk RNA-Seq demonstrated significant alterations in metabolic and inflammatory pathways in the EAT of overweight/obese patients compared with lean controls. CONCLUSION: Adaptive immune cells are the predominant immune cell constituent in human EAT and SAT. The presence of underlying cardiometabolic conditions, specifically obesity and diabetes, rather than cardiac disease phenotype appears to alter the inflammatory profile of EAT. Obese states markedly alter EAT metabolic and inflammatory signaling genes, underlining the impact of obesity on the EAT transcriptome profile. FUNDING: Barts Charity MGU0413, Abbott, Medical Research Council MR/T008059/1, and British Heart Foundation FS/13/49/30421 and PG/16/79/32419. American Society for Clinical Investigation 2021-08-23 /pmc/articles/PMC8409986/ /pubmed/34283808 http://dx.doi.org/10.1172/jci.insight.145495 Text en © 2021 Vyas et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Clinical Medicine
Vyas, Vishal
Blythe, Hazel
Wood, Elizabeth G.
Sandhar, Balraj
Sarker, Shah-Jalal
Balmforth, Damian
Ambekar, Shirish G.
Yap, John
Edmondson, Stephen J.
Di Salvo, Carmelo
Wong, Kit
Roberts, Neil
Uppal, Rakesh
Adams, Ben
Shipolini, Alex
Oo, Aung Y.
Lawrence, David
Kolvekar, Shyam
Lall, Kulvinder S.
Finlay, Malcolm C.
Longhi, M. Paula
Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title_full Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title_fullStr Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title_full_unstemmed Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title_short Obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
title_sort obesity and diabetes are major risk factors for epicardial adipose tissue inflammation
topic Clinical Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8409986/
https://www.ncbi.nlm.nih.gov/pubmed/34283808
http://dx.doi.org/10.1172/jci.insight.145495
work_keys_str_mv AT vyasvishal obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT blythehazel obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT woodelizabethg obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT sandharbalraj obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT sarkershahjalal obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT balmforthdamian obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT ambekarshirishg obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT yapjohn obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT edmondsonstephenj obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT disalvocarmelo obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT wongkit obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT robertsneil obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT uppalrakesh obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT adamsben obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT shipolinialex obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT ooaungy obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT lawrencedavid obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT kolvekarshyam obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT lallkulvinders obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT finlaymalcolmc obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation
AT longhimpaula obesityanddiabetesaremajorriskfactorsforepicardialadiposetissueinflammation

Ejemplares similares