During T cell-dependent antibody responses, B cells within germinal centers (GC) alter the affinity of their antigen receptor by introducing somatic mutations into variable region of immunoglobulin (IgV) genes. During this process, GC B cells are destined to die unless positively selected by antigens and CD40-ligand. To understand survival/death control of germinal center B cell, the expression of four apoptosis-inducing genes, Fas, c-myc, Bax, and P53, together with the survival gene bcl-2, has been analyzed herein among purified tonsillar naive, GC, and memory B cells. IgD+CD38- naive B cells were separated into CD23- (mature B cell [Bm]1) subset and CD23+ (Bm2), IgD-CD38+ GC B cells were separated into subsets of CD77+ centroblasts (Bm3) and CD77- centrocytes (Bm4), whereas IgD-CD38- cells represented the Bm5 memory B cell subset. Sequence analysis of IgV region genes indicated that somatic hypermutation was triggered in the Bm3 centroblast subset. Here we show that bcl-2 is only detectable with naive (Bm1 and 2) and memory B cell (Bm5) subsets, whereas all four apoptosis-inducing genes were most significantly expressed within GC B cells. Fas was equally expressed in Bm3 centroblasts and Bm4 centrocytes, whereas Bax was most significantly expressed in Bm4 centrocytes. c-myc, a positive regulator of cell cycle, was most significantly expressed in proliferating Bm3 centroblasts, whereas P53, a negative regulator of cell cycle, was most signficantly expressed in nonproliferating Bm4 centrocytes. The present results indicate that the survival/death of GC B cells are regulated by the up- and downregulation of multiple genes, among which the expression of c-myc and P53 in the absence of bcl-2 may prime the proliferating Bm3 centroblasts and nonproliferating Bm4 centrocytes to apoptosis.
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1 March 1996
Article|
March 01 1996
Human germinal center B cells express the apoptosis-inducing genes Fas, c-myc, P53, and Bax but not the survival gene bcl-2.
H Martinez-Valdez,
H Martinez-Valdez
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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C Guret,
C Guret
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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O de Bouteiller,
O de Bouteiller
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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I Fugier,
I Fugier
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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J Banchereau,
J Banchereau
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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Y J Liu
Y J Liu
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
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H Martinez-Valdez
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
C Guret
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
O de Bouteiller
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
I Fugier
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
J Banchereau
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
Y J Liu
Schering-Plough, Laboratory for Immunological Research, Dardilly, France.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1996) 183 (3): 971–977.
Citation
H Martinez-Valdez, C Guret, O de Bouteiller, I Fugier, J Banchereau, Y J Liu; Human germinal center B cells express the apoptosis-inducing genes Fas, c-myc, P53, and Bax but not the survival gene bcl-2.. J Exp Med 1 March 1996; 183 (3): 971–977. doi: https://doi.org/10.1084/jem.183.3.971
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