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Spi-B inhibits human plasma cell differentiation by repressing BLIMP1 and XBP-1 expression.


ABSTRACT: The terminal differentiation of B cells into antibody-secreting plasma cells is tightly regulated by a complex network of transcription factors. Here we evaluated the role of the Ets factor Spi-B during terminal differentiation of human B cells. All mature tonsil and peripheral blood B-cell subsets expressed Spi-B, with the exception of plasma cells. Overexpression of Spi-B in CD19(+) B cells inhibited, similar to the known inhibitor BCL-6, the expression of plasma cell-associated surface markers and transcription factors as well as immunoglobulin production, ie, in vitro plasma cell differentiation. The arrest in B-cell differentiation enforced by Spi-B was independent of the transactivation domain, but dependent on the Ets-domain. By chromatin immunoprecipitation and assays using an inducible Spi-B construct BLIMP1 and XBP-1 were identified as direct target genes of Spi-B mediated repression. We propose a novel role for Spi-B in maintenance of germinal center and memory B cells by direct repression of major plasma cell factors and thereby plasma cell differentiation.

SUBMITTER: Schmidlin H 

PROVIDER: S-EPMC2518887 | biostudies-other | 2008 Sep

REPOSITORIES: biostudies-other

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Spi-B inhibits human plasma cell differentiation by repressing BLIMP1 and XBP-1 expression.

Schmidlin Heike H   Diehl Sean A SA   Nagasawa Maho M   Scheeren Ferenc A FA   Schotte Remko R   Uittenbogaart Christel H CH   Spits Hergen H   Blom Bianca B  

Blood 20080613 5


The terminal differentiation of B cells into antibody-secreting plasma cells is tightly regulated by a complex network of transcription factors. Here we evaluated the role of the Ets factor Spi-B during terminal differentiation of human B cells. All mature tonsil and peripheral blood B-cell subsets expressed Spi-B, with the exception of plasma cells. Overexpression of Spi-B in CD19(+) B cells inhibited, similar to the known inhibitor BCL-6, the expression of plasma cell-associated surface marker  ...[more]

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