ERG Controls B Cell Development by Promoting Igh V-to-DJ Recombination

Elisabeth Søndergaard, Alexander Rauch, Magali Michaut, Nicolas Rapin, Matilda Rehn, Anna S. Wilhelmson, Alessandro Camponeschi, Marie S. Hasemann, Frederik O. Bagger, Johan Jendholm, Kasper J. Knudsen, Susanne Mandrup, Inga Lill Mårtensson, Bo T. Porse*

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Abstract

B cell development depends on the coordinated expression and cooperation of several transcription factors. Here we show that the transcription factor ETS-related gene (ERG) is crucial for normal B cell development and that its deletion results in a substantial loss of bone marrow B cell progenitors and peripheral B cells, as well as a skewing of splenic B cell populations. We find that ERG-deficient B lineage cells exhibit an early developmental block at the pre-B cell stage and proliferate less. The cells fail to express the immunoglobulin heavy chain due to inefficient V-to-DJ recombination, and cells that undergo recombination display a strong bias against incorporation of distal V gene segments. Furthermore, antisense transcription at PAX5-activated intergenic repeat (PAIR) elements, located in the distal region of the Igh locus, depends on ERG. These findings show that ERG serves as a critical regulator of B cell development by ensuring efficient and balanced V-to-DJ recombination.
OriginalsprogEngelsk
TidsskriftCell Reports
Vol/bind29
Udgave nummer9
Sider (fra-til)2756-2769.e6
Antal sider21
ISSN2211-1247
DOI
StatusUdgivet - 26. nov. 2019

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