B cell receptor signal strength determines B cell fate

Casola, S.; Otipoby, K.L.; Alimzhanov, M.; Humme, S.; Uyttersprot, N.; Kutok, J.L.; Carroll, M.C.; Rajewsky, K.

doi:10.1038/ni1036

B cell receptor (BCR)-mediated antigen recognition is thought to regulate B cell differentiation. BCR signal strength may also influence B cell fate decisions. Here, we used the Epstein-Barr virus protein LMP2A as a constitutively active BCR surrogate to study the contribution of BCR signal strength in B cell differentiation. Mice carrying a targeted replacement of Igh by LMP2A leading to high or low expression of the LMP2A protein developed B-1 or follicular and marginal zone B cells, respectively. These data indicate that BCR signal strength, rather than antigen specificity, determines mature B cell fate. Furthermore, spontaneous germinal centers developed in gut-associated lymphoid tissue of LMP2A mice, indicating that microbial antigens can promote germinal centers independently of BCR-mediated antigen recognition.

B cell receptor signal strength determines B cell fate / S. Casola, K.L. Otipoby, M. Alimzhanov, S. Humme, N. Uyttersprot, J.L. Kutok, M.C. Carroll, K. Rajewsky. - In: NATURE IMMUNOLOGY. - ISSN 1529-2908. - 5:3(2004), pp. 317-327. [10.1038/ni1036]

B cell receptor signal strength determines B cell fate

S. Casola^Primo;Otipoby K. L.;Alimzhanov M.;Humme S.;Uyttersprot N.;Kutok J. L.;Carroll M. C.;Rajewsky K.

2004

Abstract

B cell receptor (BCR)-mediated antigen recognition is thought to regulate B cell differentiation. BCR signal strength may also influence B cell fate decisions. Here, we used the Epstein-Barr virus protein LMP2A as a constitutively active BCR surrogate to study the contribution of BCR signal strength in B cell differentiation. Mice carrying a targeted replacement of Igh by LMP2A leading to high or low expression of the LMP2A protein developed B-1 or follicular and marginal zone B cells, respectively. These data indicate that BCR signal strength, rather than antigen specificity, determines mature B cell fate. Furthermore, spontaneous germinal centers developed in gut-associated lymphoid tissue of LMP2A mice, indicating that microbial antigens can promote germinal centers independently of BCR-mediated antigen recognition.

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				Settore MEDS-02/A - Patologia generale
			
	Data di pubblicazione
	
				2004
			
	Rivista in ANCE
	
				NATURE IMMUNOLOGY
			
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				https://dx.doi.org/10.1038/ni1036
			
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1157826

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