Affiliation:
1. Department of Physiology and Cell Biology Dorothy M. Davis Heart and Lung Institute Wexner Medical Center College of Medicine The Ohio State University Columbus OH
2. Department of Microbial Infection and Immunity Center for Microbial Interface Biology Wexner Medical Center College of Medicine The Ohio State University Columbus OH
3. Division of Pulmonary Critical Care and Sleep Medicine Department of Internal Medicine Wexner Medical Center College of Medicine The Ohio State University Columbus OH
4. Department of Emergency Medicine Department of Physiology and Cell Biology College of Medicine The Ohio State University Columbus OH
Abstract
Background
Sepsis patients with cardiac dysfunction have significantly higher mortality. Although several pathways are associated with myocardial damage in sepsis, the precise cause(s) remains unclear and treatment options are limited. This study was designed to develop a new model to investigate the early events of cardiac damage during sepsis progression.
Methods and Results
Francisella tularensis subspecies novicida
(
Ft.n
) is a Gram‐negative intracellular pathogen causing severe sepsis syndrome in mice.
BALB
/c mice (N=12) were sham treated or infected with
Ft.n
through the intranasal route. Serial electrocardiograms were recorded at multiple time points until 96 hours. Hearts were then harvested for histology and gene expression studies. Similar to septic patients, we illustrate both cardiac electrical and structural phenotypes in our murine
Ft.n
infection model, including prominent R' wave formation, prolonged
QRS
intervals, and significant left ventricular dysfunction. Notably, in infected animals, we detected numerous microlesions in the myocardium, previously observed following nosocomial
Streptococcu
s infection and in sepsis patients. We show that
Ft.n
‐mediated microlesions are attributed to cardiomyocyte apoptosis, increased immune cell infiltration, and expression of inflammatory mediators (tumor necrosis factor, interleukin [
IL]
‐1β,
IL
‐8, and superoxide dismutase 2). Finally, we identify increased expression of microRNA‐155 and rapid degradation of heat shock factor 1 following cardiac
Ft.n
infection as a primary cause of myocardial inflammation and apoptosis.
Conclusions
We have developed and characterized an
Ft.n
infection model to understand the pathogenesis of cardiac dysregulation in sepsis. Our findings illustrate novel in vivo phenotypes underlying cardiac dysfunction during
Ft.n
infection with significant translational impact on our understanding of sepsis pathophysiology.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Cardiology and Cardiovascular Medicine
Cited by
30 articles.
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