Novel Vaccine Candidates against Brucella melitensis Identified through Reverse Vaccinology Approach
Global health therapeutics is a rapidly emerging facet of postgenomics medicine. In this connection, Brucella melitensis is an intracellular bacterium that causes the zoonotic infectious disease, brucellosis. Presently, no licensed vaccines are available for human brucellosis. Here, we report the id...
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Veröffentlicht in: | Omics (Larchmont, N.Y.) N.Y.), 2015-11, Vol.19 (11), p.722-729 |
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Zusammenfassung: | Global health therapeutics is a rapidly emerging facet of postgenomics medicine. In this connection,
Brucella melitensis
is an intracellular bacterium that causes the zoonotic infectious disease, brucellosis. Presently, no licensed vaccines are available for human brucellosis. Here, we report the identification of potential vaccine candidates against
B. melitensis
using a reverse vaccinology approach. Based on a systematic screening of exoproteome and secretome of
B. melitensis
16M, we identified eight proteins as potential vaccine candidates, including LPS-assembly protein LptD, a polysaccharide export protein, a cell surface protein, heme transporter BhuA, flagellin FliC, 7-alpha-hydroxysteroid dehydrogenase, immunoglobulin-binding protein EIBE, and hemagglutinin. Among these, the roles of BhuA and hemagglutinin in the virulence of
Brucella
are essential to establish infection. Roles of other proteins in the virulence are yet to be studied. Prediction of protein–protein interactions revealed that these proteins can interact with other proteins involved in virulence, secretion system, metabolism, and transport. From these eight potential vaccine candidates, we predicted three surface exposed novel antigenic epitopes that can induce both B-cell and T-cell immune responses. These peptides can be used for the development of either exclusive peptide vaccines or multi-component vaccines against human brucellosis. Reverse vaccinology is an important strategy for discovery of novel global health therapeutics. |
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ISSN: | 1536-2310 1557-8100 |
DOI: | 10.1089/omi.2015.0105 |