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CTCF orchestrates the germinal centre transcriptional program and prevents premature plasma cell differentiation.


ABSTRACT: In germinal centres (GC) mature B cells undergo intense proliferation and immunoglobulin gene modification before they differentiate into memory B cells or long-lived plasma cells (PC). GC B-cell-to-PC transition involves a major transcriptional switch that promotes a halt in cell proliferation and the production of secreted immunoglobulins. Here we show that the CCCTC-binding factor (CTCF) is required for the GC reaction in vivo, whereas in vitro the requirement for CTCF is not universal and instead depends on the pathways used for B-cell activation. CTCF maintains the GC transcriptional programme, allows a high proliferation rate, and represses the expression of Blimp-1, the master regulator of PC differentiation. Restoration of Blimp-1 levels partially rescues the proliferation defect of CTCF-deficient B cells. Thus, our data reveal an essential function of CTCF in maintaining the GC transcriptional programme and preventing premature PC differentiation.

SUBMITTER: Perez-Garcia A 

PROVIDER: S-EPMC5504274 | biostudies-literature | 2017 Jul

REPOSITORIES: biostudies-literature

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CTCF orchestrates the germinal centre transcriptional program and prevents premature plasma cell differentiation.

Pérez-García Arantxa A   Marina-Zárate Ester E   Álvarez-Prado Ángel F ÁF   Ligos Jose M JM   Galjart Niels N   Ramiro Almudena R AR  

Nature communications 20170705


In germinal centres (GC) mature B cells undergo intense proliferation and immunoglobulin gene modification before they differentiate into memory B cells or long-lived plasma cells (PC). GC B-cell-to-PC transition involves a major transcriptional switch that promotes a halt in cell proliferation and the production of secreted immunoglobulins. Here we show that the CCCTC-binding factor (CTCF) is required for the GC reaction in vivo, whereas in vitro the requirement for CTCF is not universal and in  ...[more]

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