TY - JOUR
T1 - The capsular polysaccharide Vi from Salmonella typhi is a B1b antigen
AU - Marshall, Jennifer L.
AU - Flores-Langarica, Adriana
AU - Kingsley, Robert A.
AU - Hitchcock, Jessica R.
AU - Ross, Ewan A.
AU - López-Macías, Constantino
AU - Lakey, Jeremy
AU - Martin, Laura B.
AU - Toellner, Kai Michael
AU - MacLennan, Calman A.
AU - MacLennan, Ian C.
AU - Henderson, Ian R.
AU - Dougan, Gordon
AU - Cunningham, Adam F.
PY - 2012/12/15
Y1 - 2012/12/15
N2 - Vaccination with purified capsular polysaccharide Vi Ag from Salmonella typhi can protect against typhoid fever, although the mechanism for its efficacy is not clearly established. In this study, we have characterized the B cell response to this vaccine in wild-type and T cell-deficient mice. We show that immunization with typhoid vi polysaccharide vaccine rapidly induces proliferation in B1b peritoneal cells, but not in B1a cells or marginal zone B cells. This induction of B1b proliferation is concomitant with the detection of splenic Vi-specific Ab-secreting cells and protective Ab in Rag1-deficient B1b cell chimeras generated by adoptive transfer-induced specific Ab after Vi immunization. Furthermore, Ab derived from peritoneal B cells is sufficient to confer protection against Salmonella that express Vi Ag. Expression of Vi by Salmonella during infection did not inhibit the development of early Ab responses to non-Vi Ags. Despite this, the protection conferred by immunization of mice with porin proteins from Salmonella, which induce Ab-mediated protection, was reduced postinfection with Vi-expressing Salmonella, although protection was not totally abrogated. This work therefore suggests that, in mice, B1b cells contribute to the protection induced by Vi Ag, and targeting non-Vi Ags as subunit vaccines may offer an attractive strategy to augment current Vi-based vaccine strategies.
AB - Vaccination with purified capsular polysaccharide Vi Ag from Salmonella typhi can protect against typhoid fever, although the mechanism for its efficacy is not clearly established. In this study, we have characterized the B cell response to this vaccine in wild-type and T cell-deficient mice. We show that immunization with typhoid vi polysaccharide vaccine rapidly induces proliferation in B1b peritoneal cells, but not in B1a cells or marginal zone B cells. This induction of B1b proliferation is concomitant with the detection of splenic Vi-specific Ab-secreting cells and protective Ab in Rag1-deficient B1b cell chimeras generated by adoptive transfer-induced specific Ab after Vi immunization. Furthermore, Ab derived from peritoneal B cells is sufficient to confer protection against Salmonella that express Vi Ag. Expression of Vi by Salmonella during infection did not inhibit the development of early Ab responses to non-Vi Ags. Despite this, the protection conferred by immunization of mice with porin proteins from Salmonella, which induce Ab-mediated protection, was reduced postinfection with Vi-expressing Salmonella, although protection was not totally abrogated. This work therefore suggests that, in mice, B1b cells contribute to the protection induced by Vi Ag, and targeting non-Vi Ags as subunit vaccines may offer an attractive strategy to augment current Vi-based vaccine strategies.
UR - http://www.scopus.com/inward/record.url?scp=84871105323&partnerID=8YFLogxK
UR - https://www.jimmunol.org/content/189/12/5527/tab-article-info
U2 - 10.4049/jimmunol.1103166
DO - 10.4049/jimmunol.1103166
M3 - Article
C2 - 23162127
AN - SCOPUS:84871105323
SN - 0022-1767
VL - 189
SP - 5527
EP - 5532
JO - Journal of Immunology
JF - Journal of Immunology
IS - 12
ER -