par Marechal, Yoann 
;Queant, Séverine ;Polizzi, Selena ;Pouillon, Valérie ;Schurmans, Stéphane
Référence Immunobiology, 216, 1-2, page (103-109)
Publication Publié, 2011
;Queant, Séverine ;Polizzi, Selena ;Pouillon, Valérie ;Schurmans, Stéphane Référence Immunobiology, 216, 1-2, page (103-109)
Publication Publié, 2011
Article révisé par les pairs
| Résumé : | Inositol 1,4,5-trisphosphate 3-kinase B (or Itpkb) and inositol 1,3,4,5-tetrakisphosphate (Ins(1,3,4,5)P4), its reaction product, play an important role in the control of B lymphocyte fate and function in vivo. In order to investigate the fine mechanisms of Itpkb and Ins(1,3,4,5)P4 action in B cells, we crossed Itpkb(-/-) mice with transgenic mice expressing a 3-83μδ B cell receptor (BCR) specific for membrane-bound MHC-I H2-K(b) and H2-K(k) molecules. On a non-deleting H2-K(d) genetic background, we show that Itpkb is important for the control of Bim protein expression and B cell survival rather than for the control of B cell development from one stage to another. Analyses of cell surface markers expression, proapoptotic Bim protein expression, in vitro survival and in vivo turnover demonstrated that BCR transgenic Itpkb(-/-) B cells exhibit an anergic phenotype with the notable exception of their enhanced antigen-induced calcium signalling. On a deleting H2-K(b) genetic background, we show that Itpkb is not essential for BCR editing or negative selection. These data establish Itpkb as an important regulator of B cell survival and anergy in vivo. |
