An Erg driven transcriptional program controls B-lymphopoiesis

Author:

Ng Ashley P.ORCID,Coughlan Hannah D.ORCID,Hediyeh-zadeh SoroorORCID,Behrens Kira,Johanson Timothy M.,Yuan Low Michael SzeORCID,Bell Charles C.ORCID,Gilan OmerORCID,Chan Yih-Chih,Kueh Andrew J.,Boudier ThomasORCID,DiRago Ladina,Hyland Craig D.,Ierino Helen,Mifsud Sandra,Viney Elizabeth,Willson Tracy,Dawson Mark A.ORCID,Allan Rhys S.ORCID,Herold Marco J.ORCID,Rogers KellyORCID,Tarlinton David MORCID,Smyth Gordon K.ORCID,Davis Melissa J.ORCID,Nutt Stephen L.ORCID,Alexander Warren S.

Abstract

Summary/AbstractB-cell development is initiated by the stepwise differentiation of hematopoietic stem cells into lineage committed progenitors, ultimately generating the mature B-cells that mediate protective immunity. This highly regulated process also generates clonal immunological diversity via recombination of immunoglobulin genes. While several transcription factors that control B-cell development and V(D)J recombination have been defined, how these processes are initiated and coordinated into a precise regulatory network remains poorly understood. Here, we show that the transcription factor ETS Related Gene (Erg) is essential for the earliest steps in B-cell differentiation. Erg initiates a transcriptional network involving the B-cell lineage defining genes, Ebf1 and Pax5, that directly promotes the expression of key genes involved in V(D)J recombination and formation of the B-cell receptor. Complementation of the Erg-deficiency with a productively rearranged immunoglobulin gene rescued B-cell development, demonstrating that Erg is an essential and exquisitely stage specific regulator of the gene regulatory network controlling B-lymphopoiesis.

Publisher

Cold Spring Harbor Laboratory

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