IgG and IgG2 antibodies from cattle naturally infected with Anaplasma marginale recognize the recombinant vaccine candidate antigens VirB9, VirB10, and elongation factor-Tu
Anaplasma marginale is an important vector-borne rickettsia of ruminants in tropical and subtropical regions of the world. Immunization with purified outer membranes of this organism induces protection against acute anaplasmosis. Previous studies, with proteomic and genomic approach identified 21 pr...
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Veröffentlicht in: | Memórias do Instituto Oswaldo Cruz 2008-03, Vol.103 (2), p.186-190 |
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Zusammenfassung: | Anaplasma marginale is an important vector-borne rickettsia of
ruminants in tropical and subtropical regions of the world.
Immunization with purified outer membranes of this organism induces
protection against acute anaplasmosis. Previous studies, with proteomic
and genomic approach identified 21 proteins within the outer membrane
immunogen in addition to previously characterized major surface
protein1a-5 (MSP1a-5). Among the newly described proteins were VirB9,
VirB10, and elongation factor-Tu (EF-Tu). VirB9, VirB10 are considered
part of the type IV secretion system (TFSS), which mediates secretion
or cell-to-cell transfer of macromolecules, proteins, or DNA-protein
complexes in Gram-negative bacteria. EF-Tu can be located in the
bacterial surface, mediating bacterial attachment to host cells, or in
the bacterial cytoplasm for protein synthesis. However, the roles of
VirB9, VirB10, and TFSS in A. marginale have not been defined. VirB9,
VirB10, and EF-Tu have not been explored as vaccine antigens. In this
study, we demonstrate that sera of cattle infected with A. marginale,
with homologous or heterologous isolates recognize recombinant VirB9,
VirB10, and EF-Tu. IgG2 from naturally infected cattle also reacts with
these proteins. Recognition of epitopes by total IgG and by IgG2 from
infected cattle with A. marginale support the inclusion of these
proteins in recombinant vaccines against this rickettsia. |
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ISSN: | 1678-8060 0074-0276 0074-0276 1678-8060 |
DOI: | 10.1590/S0074-02762008000200010 |