Pneumonia Clinical Trial
Official title:
Humoral Determinants of Immunity to Pneumococcal Infection
The purpose of this study is to determine whether there are differences in the level of antibody to capsular polysaccharides of S. pneumoniae or the physiological activity of such antibody after vaccinating patients who have recovered from pneumococcal pneumonia with pneumococcal polysaccharide vaccine (Pneumovax) or conjugate pneumococcal vaccine (Prevnar).
Streptococcus pneumoniae (pneumococcus) is the most common cause of pneumonia leading to
hospitalization of adults. Resistance to infection is generally thought to be highly
associated with antibody to the capsular polysaccharide (CPS). Most people who develop
pneumococcal pneumonia lack antibody to the capsule of the infecting type. We have previously
shown that some persons develop this infection despite the presence of antibody to the
capsular polysaccharide of the infecting type. When such antibody is found, it tends to be
poorly functional (DM Musher et al, J Infect Dis 182:158-167, 2000) in that it opsonizes
pneumococci poorly for phagocytosis by human white blood cells in vitro, and protects mice
poorly or not at all against challenge with the infecting organism.
About 20% of patients with pneumococcal pneumonia in our previous study had been vaccinated
with the only vaccine currently in use for adults, namely 23-valent pneumococcal vaccine
(Pneumovax [Merck]). This product consists of purified capsular polysaccharides from 23
different serotypes of S. pneumoniae. During the past two years, with more active vaccination
programs at our hospital, the proportion of pneumococcal pneumonia patients who have been
vaccinated has increased to about 60%. Clearly, the vaccine has not provided a full degree of
protection.
After many years of study, including one involving nearly 40,000 children in the Kaiser
Permanent health care system, a new form of pneumococcal vaccine was released. In this
vaccine, Prevnar [Wyeth-Lederle], capsular polysaccharide from 7 of the most common
pneumococcal types were conjugated to a protein that closely resembles diphtheria toxoid.
There have been suggestions that Prevnar stimulates antibody in some subjects who fail to
respond to Pneumovax (DM Musher et al, Clin Infect Dis 27:1487-1490, 1998) and also that the
resulting antibody may more effectively opsonize bacteria for phagocytosis.
We propose to focus the present research on persons who develop pneumococcal pneumonia, a
group that is regarded as being at very high risk of reinfection. Persons who recover from
pneumococcal pneumonia will be randomized to vaccination revaccination with Pneumovax or
vaccination with Prevnar. These studies will clarify whether administration of protein
conjugate pneumococcal vaccine stimulates antibody in patients with pneumonia who failed to
respond to prior vaccination or stimulates better functional antibody in those who have
previously responded with antibody that is only poorly functional.
Our laboratory and others have shown that Prevnar successfully immunizes adults (Ahmed et al,
J Infect Dis 173:83-90, 1996). The vaccine is not officially recommended for adults because
antibody levels are the same after Prevnar as after Pneumovax. Such antibody may be more
functional; this has not yet been determined. Prevnar contains only 7 antigens whereas
Pneumovax contains 23 antigens; thus, it would be less desirable, in general, to administer
this vaccine instead of Pneumovax. However, in patients who have developed pneumonia despite
having received Pneumovax, the conjugate vaccine may offer an opportunity to stimulate
production of effective antibody. In the proposed research, all participants will eventually
receive both Pneumovax and Prevnar.
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