Mucosa-Associated Epithelial Chemokine/CCL28 Expression in the Uterus Attracts CCR10+ IgA Plasma Cells following Mucosal Vaccination via Estrogen Control

Abstract: Previous studies demonstrated cross talk between mucosal and reproductive organs during secretory IgA Ab induction. In this study, we aimed to clarify the underlying mechanisms of this cross talk. We found significantly higher titers of Ag-specific secretory IgA Ab in the vaginal wash after mucosal vaccination by both the intranasal (i.n.) and the intravaginal routes but not by the s.c. route. Interestingly, Ag-specific IgA Ab-secreting cells (ASCs) were found mainly in the uterus but not in the cervix and vag… Show more

“…However, the vaginal IgA is from both systemic and local production (97). The IgA levels in the genital tract are subject to a strong hormonal control that regulates the transportation of immunoglobulins, the level of cytokines, the distribution of various cell populations, and antigen presentation during the reproductive cycle as well as a compartmentalization of the immune response within the genital tract (97,98). All these factors may affect the level of IgA at a given time point.…”

A Colanic Acid Operon Deletion Mutation Enhances Induction of Early Antibody Responses by Live Attenuated Salmonella Vaccine Strains

“…However, the vaginal IgA is from both systemic and local production (97). The IgA levels in the genital tract are subject to a strong hormonal control that regulates the transportation of immunoglobulins, the level of cytokines, the distribution of various cell populations, and antigen presentation during the reproductive cycle as well as a compartmentalization of the immune response within the genital tract (97,98). All these factors may affect the level of IgA at a given time point.…”

A Colanic Acid Operon Deletion Mutation Enhances Induction of Early Antibody Responses by Live Attenuated Salmonella Vaccine Strains

“…This is thought to be the reason why vaccine administration at sites other than the mucosa is generally ineffective at promoting mucosal immunity [36]. The imprinting of gut homing molecules on lymphocytes by DCs is dependent on retinoic acid [76][77][78]. Upon antigen encounter, CD103 + DCs undergo maturation which allows them to migrate to the MLNs, initiating adaptive immune responses [73] ( Fig.…”

Delivery strategies to enhance oral vaccination against enteric infections

“…This is achieved by particular combinations of specific combinations of chemokine receptors (CCR9, CCR10, CXCR3, CXCR4) and adhesion molecules (α4β7 and α4β1) that are programmed at the same time as mucosal IgA induction (Bowman et al, 2002;Lazarus et al, 2003;Hieshima et al, 2004;Jaimes et al, 2004;Wilson and Butcher, 2004;Mora et al, 2006;Mora and Von Andrian, 2008;Morteau et al, 2008;Cha et al, 2011;Agnello et al, 2013).…”

The Regulation of IgA Production