Vaccine Induced Immune-Inflammatory Response and Cardiovascular Risk
Project Number5R01HL151828-04
Former Number1R01HL151828-01
Contact PI/Project LeaderCHENG, SUSAN
Awardee OrganizationCEDARS-SINAI MEDICAL CENTER
Description
Abstract Text
Project Summary
In the midst of emerging threats from sporadic viral entities, the perennial influenza viral strains continue to
impose a substantial burden of morbidity and mortality that compounds total annual risks to the population at
large. Last season (2018-19), influenza affected 35.5 million and led to 490,600 hospitalizations and 34,200
deaths in the U.S. These vital statistics have been steadily rising each year. Individuals with cardiovascular
disease are especially susceptible to the morbidity and mortality associated community-acquired viral
infections such as influenza. Vaccination significantly reduces the incidence of cardiovascular events at the
population level; However, administration of influenza vaccination at the individual level is extremely variable
with respect to (i) the extent of humoral antibody response achieved, and (ii) the degree of cardioprotection
conferred. Intriguingly, the degree of cardioprotection conferred does not depend entirely on the level of
humoral immunity achieved, highlighting further opportunities to discover and derive clinical benefit from a
preventive therapy with both complex and non- uniform effects. Accumulating evidence now indicates that
upstream mediators of endogenous immune- inflammatory pathways are likely key determinants of the
individual-level response to and benefit from an administered vaccination. These molecular mediators of
systemic immune-inflammatory activity, termed eicosanoids, include a diverse family of small bioactive lipids
that are enzymatically derived from polyunsaturated fatty acids. Based on results from preliminary studies, we
hypothesize that specific eicosanoids not only predict the immunologic response to influenza vaccination but
also predict its conferred protection from adverse cardiovascular events, irrespective of infection status.
Therefore, we propose an ancillary study for the NHLBI-funded INfluenza Vaccine to Effectively Stop
cardioThoracic Events and Decompensated heart failure (INVESTED) trial, that aims to: (1) identify
eicosanoids that predict the classic humoral antibody response to influenza vaccination in patients with
chronic cardiovascular disease, who represent the population subset most at-risk for adverse events; and,
(2) identify eicosanoids generated in response to vaccination that correspond with reduced risk for
cardiovascular events, irrespective of humoral immunity and infection status. The existing infrastructure of
the INVESTED trial offers a cost-effective way to reach individuals who are at the highest risk for influenza-
associated events and enable a rigorous study design for investigating heterogeneity in the response to and
benefit from vaccination.
Public Health Relevance Statement
Project Narrative
Influenza related morbidity and mortality continues to steadily increase each year, and the persons most at
risk include those with cardiovascular disease. Vaccination reduces the incidence of cardiovascular events at
the population level, but the degree of immunoprotection and cardioprotection achieved at the individual level
is highly variable. We will investigate the extent to which upstream immune-inflammatory mediators account
for individual differences in response to therapy and propensity for developing cardiovascular events.
No Sub Projects information available for 5R01HL151828-04
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