Kidney Transplant Clinical Trial
Official title:
Humoral and Cell-mediated Immune Response to Influenza Vaccine in Kidney Tranpslant Recipients.
Influenza virus is an important cause of morbidity in the transplant population and can lead to viral and bacterial pneumonia. Although the annual influenza vaccine is recommended for organ transplant patients, studies have shown that the standard inactivated influenza vaccine has poor immunogenicity in this population. One major hurdle in the evaluation of the response of influenza vaccine in immunocompromised patients is the lack of correlation between humoral response and efficacy of the vaccine. In patients with poor immune responses, cellular immunity may have a better correlation than humoral immunity with vaccine protection. We plan to assess the utility of 3 assays that evaluate the cell-mediated immune response (granzyme B, interleukin-10 (IL-10), and interferon-gamma (IFN-)) after influenza vaccine in kidney transplant recipients. Results from this study have the potential to directly improve patient care. The new monitoring assays may more accurately determine the risk for development of influenza infection, and therefore allowing a better prevention strategy.
There is limited prospective data on influenza infections in transplant recipients. However,
influenza can be a significant cause of morbidity and mortality in some organ transplant
populations. Reported attack rates have varied considerably and are likely due to
differences in transplant populations, immunosuppression protocols, exposures, and type and
virulence of circulating influenza viruses. Complications of influenza infection appear to
be common in solid organ transplant (SOT) populations. There appears to be a relatively high
rate of progression to viral pneumonia in some reports especially in lung transplant
recipients. In one study of organ transplant recipients over a 10-year period, the rate of
influenza infection ranged from 2.8 cases/1000 person years (liver transplant) to 41.8
cases/1000 person years (lung transplant). Complications including secondary bacterial
pneumonia (17%) as well as extrapulmonary complications such as myocarditis, and myositis
were observed. Influenza (and other respiratory viral infections) may lead to important
immunological sequelae resulting in graft rejection and/or graft dysfunction. This may be
secondary to activation of immunological mechanisms, including the upregulation of
pro-inflammatory cytokines such as TNF-α, IL-6 and IL-8. Some studies of kidney and liver
recipients have reported a high incidence of acute rejection following infection with
influenza. However, while associations between influenza infection and rejection have been
reported, a causal relationship has yet to be established.
Influenza vaccination has become the standard of care for several population groups. The
Centers for Disease Control and Prevention (CDC) and the Canadian National Advisory
Committee on Immunization (NACI) currently recommends this vaccine for children > 6 months,
healthy adults, the elderly and all immunocompromised patients such as those with organ
transplants (www.cdc.gov). The currently available influenza vaccine is a subunit vaccine
containing the purified surface glycoproteins of the virus, hemagglutinin and neuraminidase.
The vaccine contains 15g antigen from each of 2 circulating subtypes of influenza A and 15 g
of an influenza B subtype (www.who.int). The vaccine is administered by the intramuscular
route, generally in the deltoid muscle in adults. The standard dose is 0.5 mL.
Annual influenza vaccination is currently considered the main strategy to prevent influenza
infection for all organ transplant recipients. However, a large number of studies have shown
that the immunogenic response to this vaccine is suboptimal and ranges from 15-70%. This
number varies depending on the organ transplanted and the immunosuppressive regimen used.
Indeed, some studies in kidney transplant recipients, especially in the pediatric
population, have shown similar responses to the influenza vaccine than in healthy controls.
Monitoring of immune response to influenza vaccine. Laboratory monitoring of response to
influenza vaccine can be done by hemagglutination inhibition assay. Although laboratory
serology is a surrogate marker for protection, it is widely used. This is primarily due to
the large numbers of patients that would be needed to show vaccine efficacy if documented
influenza infection were used as the outcome. The HIA is also used by the World Health
Organization to validate annual vaccines. However, it is not known if the criteria used for
the general population may be applied in immunocompromised patients. In fact, in the elderly
it has been clearly proved that the standard cutoff for antibody levels of 40 units did not
protect against influenza. In a study with 397 elderly vaccinated against influenza, 60% of
persons who developed influenza had an antibody level of 40 units. To our knowledge, the
absolute titer of antibody required to confer significant protection from illness is unknown
in transplant patients.
Cell-mediated immunity after influenza vaccination. Recently, specific cellular responses
have also been implicated in protection against influenza, independently of the humoral
response. Cellular mediated immunity has been evaluated measuring IL-2 and IFN-(for T-helper
type 1 response), IL-10 (for T-helper type 2 response), and granzyme B expression (which
correlates with lytic activation). The cell-mediated immune response has been mainly used to
evaluate the response to influenza vaccine in the elderly. In a study with 90 persons >60
year-old, the IFN-/IL-10 ratio and granzyme B levels were significantly higher in persons
who did not develop influenza during the follow-up, compared to persons who developed
influenza. There was no correlation between the antibody levels and the risk of developing
influenza infection. In a previous study, granzyme B levels were found to be higher in young
people than in old people. Taken together, these data suggest that cell-mediated immune
response may correlate better with the risk of influenza after vaccination.
The cell-mediated immune response after influenza vaccine has been only assessed in one
study involving solid organ recipients. Mazzone et al. evaluated in 43 lung transplant
recipients and in 21 healthy controls. IL-2, IL-10, IFN-, and granzyme B levels did not
increase from pre- to post-vaccination in the lung transplant group. Both pre- and
post-cytokine levels were lower in the transplant group compared to the control group.
The study we propose is a prospective cohort trial designed to assess the immunogenicity
after a standard influenza vaccination measuring the cellular immunity in a cohort of kidney
transplant recipients, and correlate it with the standard humoral immunity.
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