It is particularly useful when comparison analyses across multiple models is done to produce a ‘consensus’ from the field (such as been attempted for aspects of HIV [115], HPV [114], and influenza [116] vaccine implementation). A comparison of Chlamydia screening models has been conducted [117] but currently there is only one modelling study that has assessed the potential impact and critical properties associated with Chlamydia vaccines [118]. This analysis

considered not only the public health outcomes of vaccine implementation but the measurable biological properties to be assessed in vaccine design and regulation. It found that in order to have the greatest public health impact, a vaccine should primarily aim to increase the threshold of the infectious dose required to infect susceptible individuals. this website The next most important objective SCR7 supplier would be to decrease the peak infectiousness among infected individuals.

Both these parameters are regularly measured in vaccine trials (in the mouse model) and several vaccine antigens are showing promise in this regard. The duration of vaccine efficacy was also identified to be of large importance and would influence the coverage and boosting schedule required in implementation to achieve a desired epidemiological outcome. This is one aspect that has not yet been well addressed in vaccine trials. But an imperfect vaccine second can still have an impact. For example, a vaccine which reduces the peak chlamydial load among infected individuals by just 1 − log10 could reduce prevalence of Chlamydia in the population by 40–50% after 20 years. In this respect, the models are very useful in that they give us an idea of just how effective a vaccine needs to be to (i.e. what level of infectious load reduction) when translating mouse model data eventually across to human population studies. While progress towards an effective C. trachomatis vaccine has been reasonably slow, it nevertheless

has moved forward in a stepwise fashion, and there are some recent events that could significantly accelerate this goal. Whole organism vaccines (whether live or inactivated) do show a significant degree of protection, usually far beyond that obtained by individual purified antigen vaccines. Therefore, if we can avoid the deleterious pathology associated with these earlier versions, perhaps we can use this general approach. In this respect, the recent Libraries findings that the chlamydial plasmid contributes, by an as yet undefined mechanism, to the adverse pathology observed in both C. trachomatis and C. muridarum infections, could be a major opportunity [119]. A plasmid-free, attenuated strain of C.