STAT5 regulates the self-renewal capacity and differentiation of human memory B cells and controls Bcl-6 expression

Ferenc A. Scheeren; Marianne Naspetti; Sean Diehl; Remko Schotte; Maho Nagasawa; Erwin Wijnands; Ramon Gimeno; Florry A. Vyth-Dreese; Bianca Blom; Hergen Spits

doi:https://doi.org/10.1038/ni1172

STAT5 regulates the self-renewal capacity and differentiation of human memory B cells and controls Bcl-6 expression

Ferenc A. Scheeren, Marianne Naspetti, Sean Diehl, Remko Schotte, Maho Nagasawa, Erwin Wijnands, Ramon Gimeno, Florry A. Vyth-Dreese, Bianca Blom, Hergen Spits

Research output: Contribution to journal › Article › Academic › peer-review

136 Citations (Scopus)

Abstract

It is unknown how B cells that mature during a germinal center reaction 'decide' between plasma or memory cell fate. Here we describe a previously unknown subpopulation of B cells in the human germinal center that is characterized by tyrosine phosphorylated transcriptional activator STAT5. These cells had an activated centrocyte phenotype and had abundant expression of BCL6 but low expression of PRDM1, both encoding transcriptional repression proteins. Using RNA interference and ectopic expression of constitutively activated forms of STAT5, we demonstrate here a function for STAT5 in the self-renewal of B cells in vitro. STAT5b isoform seemed to directly upregulate Bcl-6, and ectopic expression of Bcl-6 in B cells resulted in self-renewal and inhibition of plasma cell differentiation. These data indicate that activation of STAT5 is involved in regulation of memory B cell differentiation

Original language	English
Pages (from-to)	303-313
Journal	Nature immunology
Volume	6
Issue number	3
DOIs	https://doi.org/10.1038/ni1172
Publication status	Published - 2005

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https://doi.org/10.1038/ni1172

Cite this

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title = "STAT5 regulates the self-renewal capacity and differentiation of human memory B cells and controls Bcl-6 expression",

abstract = "It is unknown how B cells that mature during a germinal center reaction 'decide' between plasma or memory cell fate. Here we describe a previously unknown subpopulation of B cells in the human germinal center that is characterized by tyrosine phosphorylated transcriptional activator STAT5. These cells had an activated centrocyte phenotype and had abundant expression of BCL6 but low expression of PRDM1, both encoding transcriptional repression proteins. Using RNA interference and ectopic expression of constitutively activated forms of STAT5, we demonstrate here a function for STAT5 in the self-renewal of B cells in vitro. STAT5b isoform seemed to directly upregulate Bcl-6, and ectopic expression of Bcl-6 in B cells resulted in self-renewal and inhibition of plasma cell differentiation. These data indicate that activation of STAT5 is involved in regulation of memory B cell differentiation",

author = "Scheeren, {Ferenc A.} and Marianne Naspetti and Sean Diehl and Remko Schotte and Maho Nagasawa and Erwin Wijnands and Ramon Gimeno and Vyth-Dreese, {Florry A.} and Bianca Blom and Hergen Spits",

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T1 - STAT5 regulates the self-renewal capacity and differentiation of human memory B cells and controls Bcl-6 expression

AU - Scheeren, Ferenc A.

AU - Naspetti, Marianne

AU - Diehl, Sean

AU - Schotte, Remko

AU - Nagasawa, Maho

AU - Wijnands, Erwin

AU - Gimeno, Ramon

AU - Vyth-Dreese, Florry A.

AU - Blom, Bianca

AU - Spits, Hergen

PY - 2005

Y1 - 2005

N2 - It is unknown how B cells that mature during a germinal center reaction 'decide' between plasma or memory cell fate. Here we describe a previously unknown subpopulation of B cells in the human germinal center that is characterized by tyrosine phosphorylated transcriptional activator STAT5. These cells had an activated centrocyte phenotype and had abundant expression of BCL6 but low expression of PRDM1, both encoding transcriptional repression proteins. Using RNA interference and ectopic expression of constitutively activated forms of STAT5, we demonstrate here a function for STAT5 in the self-renewal of B cells in vitro. STAT5b isoform seemed to directly upregulate Bcl-6, and ectopic expression of Bcl-6 in B cells resulted in self-renewal and inhibition of plasma cell differentiation. These data indicate that activation of STAT5 is involved in regulation of memory B cell differentiation

AB - It is unknown how B cells that mature during a germinal center reaction 'decide' between plasma or memory cell fate. Here we describe a previously unknown subpopulation of B cells in the human germinal center that is characterized by tyrosine phosphorylated transcriptional activator STAT5. These cells had an activated centrocyte phenotype and had abundant expression of BCL6 but low expression of PRDM1, both encoding transcriptional repression proteins. Using RNA interference and ectopic expression of constitutively activated forms of STAT5, we demonstrate here a function for STAT5 in the self-renewal of B cells in vitro. STAT5b isoform seemed to directly upregulate Bcl-6, and ectopic expression of Bcl-6 in B cells resulted in self-renewal and inhibition of plasma cell differentiation. These data indicate that activation of STAT5 is involved in regulation of memory B cell differentiation

U2 - https://doi.org/10.1038/ni1172

DO - https://doi.org/10.1038/ni1172

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SN - 1529-2908

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