2 ELISA S/N ratio). In both these groups we observed only short-term effects with respect to proliferative responses and IFN-γ production. this website The results presented in this work indicate also that early vaccination of pigs born to immune sows with attenuated ADV vaccine leads to generation of PBMC that probably contain ADV-specific memory cells, which are characterized by a Th1-like cytokine pattern upon in vitro recall stimulation. The vaccine used in the present
study solely induced Th1-type cytokine in vitro. It was also shown that pigs vaccinated at 10 and 14 weeks of age (manufacturer’s recommendation) at the moment of first vaccination had a relatively high level of passively acquired antibodies (about 0.35 ELISA S/N ratio), but they were simultaneously able to develop an active cellular as well as humoral immunity. The duration and the intensity of the secondary proliferative responses evidenced in group 6 were even better than in group 2 (P<0.05), but weaners from this group possessed lower levels of specific antibodies from about 10 weeks of life to the end of the study. The high values of SI were also seen in pigs from group 4, but it should be noted that animals from this group had no passive protection against ADV for about 3 weeks
before vaccination. At the moment of vaccination, all weaners from this group were considered to be negative with respect to MDA, and so were in fact susceptible to infection. In practice this means that is too late to vaccinate GSK126 molecular weight at the age of 12 weeks. In the present study, besides evaluation of the influence of maternal antibodies on postvaccinal immune responses, we also wanted to estimate
the best moment for vaccination of MDA-positive pigs, taking into consideration practical and economical points of view. For example, we vaccinated the pigs once, at 8 weeks of life, to evaluate whether a single vaccination of animals at the time when they are usually introduced to the herd is enough. We also wanted to check whether earlier first vaccination (at 1 week of age) and revaccination at a later age, could be an alternative for vaccination C-X-C chemokine receptor type 7 (CXCR-7) of relatively big weaners (at 10 or 14 weeks of age), because it is easier for herd personnel to vaccinate 7-day-old piglets. Certainly there is still a need for further studies on the efficiency of vaccination with different protocols (challenge experiment) to confirm the protective effect. However, the present results allow us to exclude some protocols of vaccination from the challenge study (e.g. vaccination at 1 and 8 weeks, or at 8 weeks), reducing the number of sacrificed pigs, which is very important from an ethical point of view.