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The level of expression of mu heavy chain modifies the composition of peripheral B cell subpopulations
Authors:Sanchez P  Crain-Denoyelle A M  Daras P  Gendron M C  Kanellopoulos-Langevin C
Affiliation:Laboratoire d'Immunobiologie, Case 7048, Université Denis-Diderot (Paris 7), 2 Place Jussieu, 75251 Paris Cedex 05, France. Institut Jacques Monod, 75005 Paris, France.
Abstract:The B cell receptor (BCR) has a decisive role in transducing signals required for the development of B cells and their survival in the periphery. However, the processes that initiate these signals remain unclear and concepts of constitutive and ligand-dependent signaling have been proposed. Using a mu-transgenic mouse model, we have analyzed the impact of high surface IgM expression on the composition of the splenic B cell population. kappa-deficient mice homozygous for the H3-mu transgene have B cells with a higher BCR surface density than H3 heterozygous mice. This higher BCR expression is associated with an increase in the percentage and the total number of splenic B cells. In addition, an important proportion of CD23(-)CD21(+) marginal zone (MZ) B cells can be observed in H3 homozygous mice. However, these modifications operate in the absence of impairment of the positive selection process of the H3-mu/lambda1 combination over the H3-mu/lambda2 + 3 ones. These results suggest that (i) a constitutive BCR signaling directly correlated with BCR surface density is responsible for the efficient B cell colonization of the periphery with an accumulation of B cells in the MZ and (ii) a ligand-dependent BCR signal is responsible for the clonotype composition of the mature B cell repertoire.
Keywords:B lymphocytes, B cell repertoire,   /math/kappa.gif"   ALT="  {kappa}"   BORDER="  0"  > knockout,   /math/lambda.gif"   ALT="  {lambda}"   BORDER="  0"  > chains, µ   transgenic mice
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