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Abstract
ABSTRACTThe search for a test that can predict vaccine efficacy is an important part of any vaccine development program. Although regulators hesitate to acknowledge any test as a true ‘correlate of protection’, there are many precedents for defining ‘surrogate’ assays. Surrogates can be powerful tools for vaccine optimization, licensure, comparisons between products and development of improved products. When such tests achieve ‘reference’ status however, they can inadvertently become barriers to new technologies that do not work the same way as existing vaccines. This is particularly true when these tests are based upon circularly-defined ‘reference’ or, even worse, proprietary reagents. The situation with inactivated influenza vaccines is a good example of this phenomenon. The most frequently used tests to define vaccine-induced immunity are all serologic assays: hemagglutination inhibition (HI), single radial hemolysis (SRH) and microneutralization (MN). The first two, and particularly the HI assay, have achieved reference status and criteria have been established in many jurisdictions for their use in licensing new vaccines and to compare the performance of different vaccines. However, all of these assays are based on biological reagents that are notoriously difficult to standardize and can vary substantially by geography, by chance (i.e. developing reagents in eggs that may not antigenitically match wild-type viruses) and by intention (ie: choosing reagents that yield the most favorable results). This review describes attempts to standardize these assays to improve their performance as surrogates, the dangers of over-reliance on ‘reference’ serologic assays, the ways that manufacturers can exploit the existing regulatory framework to make their products ‘look good’ and the implications of this long-established system for the introduction of novel influenza vaccines.
Highlights
One of the ‘holy grails’ of vaccine development is the identification of an -standardized and reproducible test that can serve as an accurate predictor of vaccine efficacy across all ages and geographies: a true ‘correlate of protection’
A recent efficacy study demonstrated a 30% reduction in the risk of PCR-confirmed influenza-like illness for FluBlok compared to a standard dose of inactivated quadrivalent influenza vaccine in adults 50 years of age despite an apparent inferiority in the induction of hemagglutination inhibition (HI) antibodies for the H1N1 and B/Brisbane strains.[95]
Some of the difficulties currently confronting the influenza vaccine community were foreshadowed to some extent by Hobson’s iconic 1972 article in which an HI-based correlate of protection was proposed but which noted that subjects without any detectable HI response were better protected than those with low HI titres.[33]
Summary
One of the ‘holy grails’ of vaccine development is the identification of an -standardized and reproducible test that can serve as an accurate predictor of vaccine efficacy across all ages and geographies: a true ‘correlate of protection’.1,2 a small number of assays come close to this ideal (eg: antibody titres for hepatitis B surface antigen, bacteria toxins like tetanus or the rabies G protein), the best the vaccine community has managed in most cases is the development of ‘surrogate markers’ for immunity and protection. A small number of assays come close to this ideal (eg: antibody titres for hepatitis B surface antigen, bacteria toxins like tetanus or the rabies G protein), the best the vaccine community has managed in most cases is the development of ‘surrogate markers’ for immunity and protection. Pre-formed antibodies are critical to protect against diseases caused by bacterial toxins and can be very helpful in providing immunity against many pathogens and in preventing reinfection with the same or a related pathogen. Despite being sufficient for protection against many infectious challenges, antibodies are critically important for defense against a relatively limited number of micro-organisms: the encapsulated bacteria (Streptococcus pneumonia, the meningococci, Haemophilus influenzae), the Enteroviridae including polioviruses, some enteric bacteria (eg: Campylobacter spp.) and Giardia lamblia.[5]. Why has so much effort been placed on defining serologic surrogates of protection in vaccine development programs and in optimizing antibody responses to vaccines?
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