Post-immunization serum samples from Ty21a recipients and mononuclear cells were able to kill Salmonella Typhi, Salmonella Paratyphi A and B, but not Salmonella Paratyphi C or Salmonella
Tel Aviv, neither of which share O-antigen epitopes with Ty21a. Later, Nishini et al. [23] conducted similar experiments and found a specific cell-mediated immune response not only to Salmonella Typhi but also to Salmonella Paratyphi A and B in Ty21a recipients. This study is the first to explore cross-reactive plasmablasts in patients with typhoid or paratyphoid fever. Both specific and cross-reactive plasmablasts could be found in all of these Sorafenib cost patients. These data are in accordance with the O-/Vi-antigen properties of these pathogens. ZD1839 price In patients with typhoid fever, cross-reactive plasmablasts were seen to Salmonella Paratyphi A, B (O-12 as shared epitope in both strains) and C (Vi-antigen as shared epitope), and in the patient with paratyphoid A fever, a cross-reactive response was seen against Salmonella Typhi and Salmonella Paratyphi B (O-12 as shared epitope), but not against Salmonella Paratyphi
C (no shared epitopes). The magnitude of the response in patients and vaccinees was similar. The timing of the sampling in vaccinees was based on previous studies showing peak values of ASC seven days after vaccination [18] and [43]. In studies on natural infections, samples are taken seven days after onset of symptoms [36] and [37] as in the present study. The long incubation time in enteric fever implies that the pathogen was encountered several weeks earlier and hence, our timing may not hit the peak. However, in our recent study on Salmonella gastroenteritis, ASC were found as long as the antigen
persisted and no clear peak was seen [44]. The immunoglobulin isotype distribution of the responses in the vaccinees showed a predominance of IgA and IgM plasmablasts. This is consistent with our previous studies showing that while IgM response peaks on day 5, and IgG and IgA responses on day 7 [20], on day 7 both IgA and IgM predominate [20]. Notably, the immunoglobulin L-NAME HCl isotype switch of mucosal IgA cells may take place only after their arrival in the lamina propria, i.e. after finishing the recirculation [45]. Accordingly, when assessing mucosal immune response with the help of recirculating plasmablasts, an analysis of all three Ig-classes should always be included, as the circulating IgM-secreting plasmablasts may mature into IgA producing cells only later. This is nicely evidenced also by the fact that basically all circulating Ty21a-specific plasmablasts, regardless of isotype, express α4β7, indicating an intestinal homing of these cells [29], [30] and [40]. Our previous studies show that the numbers of plasmablasts increase with increasing numbers of Ty21a vaccine doses [20].