Validating Immunomodulatory Responses of r-<i>Ld</i>ODC Protein and Its Derived HLA-DRB1 Restricted Epitopes against Visceral Leishmaniasis in BALB/c Mice

Rajkishor Pandey; Rohit Kumar Gautam; Simran Sharma; Mebrahtu G. Tedla; Vijay Mahantesh; Manas Ranjan Dikhit; Akhilesh Kumar; Krishna Pandey; Sanjiva Bimal

doi:10.3390/pathogens12010016

Pathogens (Dec 2022)

Validating Immunomodulatory Responses of r-<i>Ld</i>ODC Protein and Its Derived HLA-DRB1 Restricted Epitopes against Visceral Leishmaniasis in BALB/c Mice

Rajkishor Pandey,
Rohit Kumar Gautam,
Simran Sharma,
Mebrahtu G. Tedla,
Vijay Mahantesh,
Manas Ranjan Dikhit,
Akhilesh Kumar,
Krishna Pandey,
Sanjiva Bimal

Affiliations

Rajkishor Pandey: Department of Biotechnology, National Institute of Pharmaceutical Education & Research, Hajipur 844102, India
Rohit Kumar Gautam: Department of Biotechnology, National Institute of Pharmaceutical Education & Research, Hajipur 844102, India
Simran Sharma: Department of Basic and Applied Sciences, National Institute of Food Technology Entrepreneurship & Management (NIFTEM), Kundli, Sonipat 131028, India
Mebrahtu G. Tedla: Department of Child Health, School of Medicine, University of Missouri-Columbia, Columbia, MO 65211, USA
Vijay Mahantesh: Department of Biotechnology, National Institute of Pharmaceutical Education & Research, Hajipur 844102, India
Manas Ranjan Dikhit: Department of Biomedical Informatics, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India
Akhilesh Kumar: Division of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India
Krishna Pandey: Department of Clinical Medicine, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India
Sanjiva Bimal: Division of Immunology, Rajendra Memorial Research Institute of Medical Sciences, Patna 800007, India

DOI: https://doi.org/10.3390/pathogens12010016
Journal volume & issue: Vol. 12, no. 1
p. 16

Abstract

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Vaccination is considered the most appropriate way to control visceral leishmaniasis (VL). With this background, the r-LdODC protein as well as its derived HLA-DRB1-restricted synthetic peptides (P1: RLMPSAHAI, P2: LLDQYQIHL, P3: GLYHSFNCI, P4: AVLEVLSAL, and P5: RLPASPAAL) were validated in BALB/c mice against visceral leishmaniasis. The study was initiated by immunization of the r-LdODC protein as well as its derived peptides cocktail with adjuvants (r-CD2 and MPL-A) in different mice groups, separately. Splenocytes isolated from the challenged and differentially immunized mice group exhibited significantly higher IFN-γ secretion, which was evidenced by the increase in the expression profile of intracellular CD4+IFN-γ T cells. However, the IL-10 secretion did not show a significant increase against the protein and peptide cocktail. Subsequently, the study confirmed the ability of peptides as immunoprophylactic agents, as the IE-I/AD-I molecule overexpressed on monocytes and macrophages of the challenged mice group. The parasitic load in macrophages of the protein and peptides cocktail immunized mice groups, and T cell proliferation rate, further established immunoprophylactic efficacy of the r-LdODC protein and peptide cocktail. This study suggests that the r-LdODC protein, as well as its derived HLA-DRB1-restricted synthetic peptides, have immunoprophylactic potential and can activate other immune cells’ functions towards protection against visceral leishmaniasis. However, a detailed study in a humanized mice model can explore its potential as a vaccine candidate.

Published in Pathogens

ISSN: 2076-0817 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine
Website: http://www.mdpi.com/journal/pathogens

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