Yellow Fever Clinical Trial
Official title:
Using Systems Vaccinology to Elucidate the Effects of Anti-inflammatory Therapy on Immune Response After Vaccination With a Live Attenuated Vaccine
Since the 1st pandemic of the 21st century caused by SARS coronavirus, the world has experienced outbreaks of swine origin H1N1 influenza, Ebola and Zika viruses, which have all resulted in global health crises. Rapid mass vaccination with an effective vaccine such as a live attenuated vaccine, of vulnerable immune-naïve populations to establish herd immunity is an approach to control outbreaks. Such live attenuated vaccine had been used with great success in sporadic yellow fever outbreaks and recently successfully employed in Ebola field trial, both of these diseases have the potential for pandemic spread. Indeed, live attenuated vaccines have proven especially effective in controlling childhood diseases and have even succeeded in eradicating polio and measles from most parts of the world. However, deployment of such vaccines for pandemic control cannot be limited to children but must include adults in order to rapidly elevate herd immunity rates to halt transmission. Vaccinating adults may produce efficacy rates significantly different to those observed in children due to the prevalence of chronic diseases and their associated metabolic complications. Presently, there are 1 billion people who are overweight, many suffer from concurrent metabolic disorders. As activation of the adaptive immunity is reliant on a robust innate immune response to vaccines, metabolic disorders and long-term anti-inflammatory therapy with interventions such as statins may reduce vaccine immunogenicity resulting in suboptimal efficacy in this subpopulation. This study would therefore test the hypothesis that statins reduce live attenuated vaccine immunogenicity. We will combine a clinical trial with systems vaccinology approaches to define the impact statins has on the innate immune, B and T-cell responses to live attenuated vaccination. Our study will thus extend upon another recently completed trial by us and will provide new insights into the determinants of vaccine efficacy in a rapidly growing and aging population globally
Despite successful control of many infectious diseases since the 19th century, viral diseases
remain an important and significant health burden in the 21st century. In fact, the turn of
the 21st century saw the emergence of not only new but also re-emergent pathogens such as
SARS, MERS, West Nile, Ebola, dengue and Zika viruses. In addition, the modern world is
highly mobile and interconnected. The spread of infectious diseases is imminently only a
flight away. It is thus of no surprise that epidemics in this century are happening at a much
faster pace and spreading quicker to cause disruption to human health, society and the
economy. Vaccination, particularly with a live attenuated vaccine (LAV), which has the most
successful track record among the various forms of vaccines, remains the most economical
public health tool available to prevent or stop the spread of infections and alleviate human
sufferings. Rapid mass vaccination of at risk populations to establish herd immunity has been
successfully employed to control sporadic YF outbreaks in Africa and South America. More
recently, a clinical trial showed that ring vaccination of contacts with Ebola patients
completely abrogated secondary virus spread. Vaccination in times of pandemics, however,
cannot be limited to children but must include adults in order to rapidly elevate herd
immunity rates to halt further transmission.
The use of LAV in adults has several important challenges that have not been systematically
addressed. The population demographics in Singapore, like most developed countries have
changed drastically over the past 3 decades. Along with improved nutrition, populations are
now living longer but with increasing prevalence of chronic diseases such as obesity and
dyslipidemia. Consequently, the anti-cholesterol group of drugs, with pleiotropic properties,
statins, are among the commonest drugs prescribed globally for the prevention of secondary
cardiovascular and major vascular complications. There is presently a mounting concern that
the anti-inflammatory and immune-modulatory effects of statins could have a detrimental
effect on vaccine efficacy. Indeed, studies examining inactivated influenza vaccination in
older individuals had observed lower immunogenicity and overall efficacy with statin use.
Whether statins have a similar negative immunogenicity effect on LAV remains undefined. The
anti-inflammatory effects may dampen innate immune responses critical for triggering adaptive
immunity resulting in reduced immunogenicity. Conversely, the suppression of innate immune
responses could favor LAV infection and replication, allowing adaptive immune cells a longer
period to sense the antigen, become activated and differentiated for improved immune
response.
In this study, an experimental medicine investigation that leverages on a recently completed
clinical trial that the PI led examining how cross-reactive antibodies altered the
immunogenicity of yellow fever (YF) vaccination. We will seek to clarify the effects of
statin on LAV immunogenicity. YF vaccine is an excellent LAV, which remains the WHO
recommended response to the ever-present threat of YF outbreak. It has also served as an
important model for studying human antiviral immunity. We propose to test the hypothesis that
long term statins therapy alters YF LAV immunogenicity by coupling the power of a clinical
trial with comprehensive systems vaccinology to define the impact statins have on the
adaptive immune response to YF vaccination. This study will elucidate how statins modulate
the networks that drive immunity to vaccination in a fast growing population globally.
Knowledge on how statins impact LAV immunogenicity would inform public health authorities on
the size of the general population that should be vaccinated to compensate for alterations in
immunogenicity in this subpopulation to achieve sufficient herd immunity for epidemic and
pandemic control.
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