Circulating Gut-Homing (α 4 β 7 + ) Plasmablast Responses against Shigella Surface Protein Antigens among Hospitalized Patients with Diarrhea

Author:

Sinha Anuradha1,Dey Ayan2,Saletti Giulietta2,Samanta Pradip1,Chakraborty Partha Sarathi1,Bhattacharya M. K.1,Ghosh Santanu1,Ramamurthy T.1,Kim Jae-Ouk2,Yang Jae Seung2,Kim Dong Wook23,Czerkinsky Cecil24,Nandy Ranjan K.1

Affiliation:

1. National Institute of Cholera and Enteric Diseases, Kolkata, India

2. International Vaccine Institute, Seoul, South Korea

3. College of Pharmacy, Hanyang University, Ansan, South Korea

4. IPMC Nice-Sophia Antipolis, Nice, France

Abstract

ABSTRACT Developing countries are burdened with Shigella diarrhea. Understanding mucosal immune responses associated with natural Shigella infection is important to identify potential correlates of protection and, as such, to design effective vaccines. We performed a comparative analysis of circulating mucosal plasmablasts producing specific antibodies against highly conserved invasive plasmid antigens (IpaC, IpaD20, and IpaD120) and two recently identified surface protein antigens, p an- S higella s urface p rotein antigen 1 (PSSP1) and PSSP2, common to all virulent Shigella strains. We examined blood and stool specimens from 37 diarrheal patients admitted to the Infectious Diseases & Beliaghata General Hospital, Kolkata, India. The etiological agent of diarrhea was investigated in stool specimens by microbiological methods and real-time PCR. Gut-homing (α 4 β 7 + ) antibody-secreting cells (ASCs) were isolated from patient blood by means of combined magnetic cell sorting and two-color enzyme-linked immunosorbent spot (ELISPOT) assay. Overall, 57% (21 of 37) and 65% (24 of 37) of the patients were positive for Shigella infection by microbiological and real-time PCR assays, respectively. The frequency of α 4 β 7 + IgG ASC responders against Ipas was higher than that observed against PSSP1 or PSSP2, regardless of the Shigella serotype isolated from these patients. Thus, α 4 β 7 + ASC responses to Ipas may be considered an indirect marker of Shigella infection. The apparent weakness of ASC responses to PSSP1 is consistent with the lack of cross-protection induced by natural Shigella infection. The finding that ASC responses to IpaD develop in patients with recent-onset shigellosis indicates that such responses may not be protective or may wane too rapidly and/or be of insufficient magnitude.

Publisher

American Society for Microbiology

Subject

Microbiology (medical),Clinical Biochemistry,Immunology,Immunology and Allergy

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