Intranasal Immunization of Mice with a Chimeric Antigen of Cholera Toxin B and Salmonella Typhi outer membrane protein T2544 elicits protective antibodies and T cell response at the intestinal mucosa

Author:

Chakraborty Suparna1,Dutta Pujarini2,Pal Ananda1,Chakraborty Swarnali1,Banik George3,Halder Prolay4,Gope Animesh4,Miyoshi Shin-ichi5,Das Santasabuj1ORCID

Affiliation:

1. ICMR- National Institute of Cholera Enteric Diseases

2. Department of Pediatrics, Steele Children’s Research Center, University of Arizona, Tuscon,Arizona

3. BD Biosciences, INDIA, Smart works Business Center, Victoria Park, 37/2 GN Block, Sector 5, Saltlake City

4. ICMR- National Institute of Cholera and Enteric Diseases,

5. Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Okayama University, Okayama Japan

Abstract

Abstract Development of safe, highly effective and affordable enteric fever vaccines is a global health priority. Live, oral typhoid vaccines induce strong mucosal immunity and long-term protection, but safety remains a concern. In contrast, efficacy wears off rapidly for injectable, polysaccharide-based vaccines, which elicit poor mucosal response. We previously reported Salmonella Typhi outer membrane protein, T2544 as a potential candidate for bivalent (S. typhi and S. Paratyphi A) vaccine development. Here, we show that intranasal immunization with a subunit vaccine (chimera of T2544 and cholera toxin B subunit) induced strong systemic and intestinal mucosal immunity and protection from S. Typhi challenge in a mouse model. CTB-T2544 augmented gut-homing receptor expression on lymphocytes that produced Th1 and Th17 cytokines, secretory IgA in stool that inhibited bacterial motility and epithelial attachment, antibody recall response and affinity maturation with increased number of follicular helper T cells and CD4 + central and effector memory cells.

Publisher

Research Square Platform LLC

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