Impact on antibody responses of B-cell-restricted transgenic expression of a viral gene inhibiting activation of NF-[kappa]B and NFAT

In this work, we have assessed the impact in vivo of the evasion gene A238L of African swine fever virus, an inhibitor of both NF-[kappa]B- and NFAT-mediated transcription. The A238L gene was selectively expressed in mouse B lymphocytes using the promoter and enhancer sequences of the mouse Ig [mu]...

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Veröffentlicht in:Archives of virology 2015-06, Vol.160 (6), p.1477
Hauptverfasser: de Paiva e Almeida, Sílvia Cristina, de Oliveira, Vivian Leite, Parkhouse, Robert Michael, Evans
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Sprache:eng
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Zusammenfassung:In this work, we have assessed the impact in vivo of the evasion gene A238L of African swine fever virus, an inhibitor of both NF-[kappa]B- and NFAT-mediated transcription. The A238L gene was selectively expressed in mouse B lymphocytes using the promoter and enhancer sequences of the mouse Ig [mu] heavy chain. The IgM primary and IgG2b secondary serological responses and the number of splenic germinal centres in response to the TD antigens DNP-keyhole limpet hemocyanin and sheep red blood cells, respectively, were both lower in the transgenic mice, whereas the response to the TI type-1 and type-2 antigens DNP-Ficoll and DNP-LPS, respectively, were normal, except for the increased levels of IgG3 at day 14 in the DNP-LPS-immunized mice. Thus, it appears that neither p65 (NF-[kappa]B) nor NFAT is essential for B-cell development but, in a manner that is still unclear, may be relevant for their function.
ISSN:0304-8608
1432-8798
DOI:10.1007/s00705-015-2419-x