Cardiac resynchronization therapy reduces expression of inflammation-promoting genes related to interleukin-1β in heart failure.

Aged Cardiac Resynchronization Therapy Cardiac Resynchronization Therapy Devices Case-Control Studies Defibrillators, Implantable Down-Regulation Electric Countershock / instrumentation Female Gene Expression Profiling Heart Failure / genetics Humans Inflammation Mediators / metabolism Interleukin-1beta / genetics Leukocytes, Mononuclear / metabolism Male Middle Aged Proto-Oncogene Mas RNA-Seq Transcriptome Treatment Outcome

Cardiac resynchronization therapy Heart failure Il-1β PCR RNA-seq

Journal

Cardiovascular research

ISSN: 1755-3245

Titre abrégé: Cardiovasc Res

Pays: England

ID NLM: 0077427

Informations de publication

Date de publication:
01 06 2020

Historique:

received: 28 01 2019

revised: 02 08 2019

accepted: 06 09 2019

pubmed: 16 10 2019

medline: 9 2 2021

entrez: 16 10 2019

Statut: ppublish

Résumé

In light of recent data regarding inflammatory signalling pathways in cardiovascular disease and the recently demonstrated impact of pharmacologic inhibition of interleukin-1β (IL-1β) in heart failure, the primary aim was to assess the physiologic effects of cardiac resynchronization therapy (CRT) on the expression of systemic inflammatory, immune-modulatory, metabolic, and apoptotic genes in peripheral blood mononuclear cells (PBMCs) of patients with heart failure. We used RNA sequencing (RNA-Seq) and reverse transcription quantitative real-time polymerase chain reaction (RT-qPCR) to identify gene expression changes in PBMCs in response to CRT. In total, 27 patients were analysed: 12 with heart failure undergoing CRT, 6 with heart failure undergoing standard implanted cardioverter defibrillators, and 9 with coronary artery disease but not heart failure. In CRT patients (median age 65.5 years, interquartile range 63.0-66.8 years, 33% female), RNA-Seq analysis identified 40 genes, including multiple genes associated with the IL-1β pathway, with significant correlations (false discovery rate < 0.05) with four key CRT response measures. CRT was associated with suppression of PBMC expression of IL-1β (1.80-fold decrease, P = 0.047), FOS proto-oncogene (FOS) (3.25-fold decrease, P = 0.01), dual specificity phosphatase 1 (DUSP1) (2.05-fold decrease, P = 0.001), and early growth response 1 (EGR1) (7.38-fold decrease, P = 0.03), and suppression was greater in responders vs. non-responders (P = 0.03 for IL-1β, P = 0.02 for FOS, P = 0.02 for DUSP1, and P = 0.11 for EGR1). Baseline FOS and DUSP-1 levels were greater in responders vs. non-responders (6.15-fold higher, FOS, P = 0.002; 2.60-fold higher, DUSP1, P = 0.0001). CRT responders but not non-responders showed higher baseline gene expression of FOS (P = 0.04) and DUSP1 (P = 0.06) compared with control patients without heart failure. Baseline serum high-sensitivity C-reactive protein levels were 3.47-fold higher in CRT responders vs. non-responders (P = 0.008). Treatment of heart failure with CRT resulted in decreased PBMC expression of genes linked to inflammation. Moreover, CRT responders had higher expression of these inflammatory genes prior to CRT and greater suppression of these genes after CRT compared with non-responders.

Identifiants

DOI: 10.1093/cvr/cvz232 PMID: 31612215 PMC: PMC7849974

pubmed: 31612215

pii: 5585796

doi: 10.1093/cvr/cvz232

pmc: PMC7849974

doi:

Substances chimiques

IL1B protein, human 0

Inflammation Mediators 0

Interleukin-1beta 0

MAS1 protein, human 0

Proto-Oncogene Mas 0

Types de publication

Comparative Study Journal Article Research Support, N.I.H., Extramural Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

Pagination

1311-1322

Subventions

Organisme : NHLBI NIH HHS

ID : R03 HL135463

Pays : United States

Organisme : NHLBI NIH HHS

ID : R56 HL135556

Pays : United States

Informations de copyright

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Cardiac resynchronization therapy reduces expression of inflammation-promoting genes related to interleukin-1β in heart failure.

Journal

Informations de publication

Résumé

Identifiants

Substances chimiques

Types de publication

Langues

Sous-ensembles de citation

Pagination

Subventions

Informations de copyright

Références

Auteurs

Kenneth Bilchick (K)

Hema Kothari (H)

Aditya Narayan (A)

James Garmey (J)

Abdullah Omar (A)

Brian Capaldo (B)

Coleen McNamara (C)

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Classifications MeSH