B-cell development fails in the absence of the Pbx1 proto-oncogene

M Sanyal, JW Tung, H Karsunky, H Zeng, L Selleri… - Blood, 2007 - ashpublications.org
M Sanyal, JW Tung, H Karsunky, H Zeng, L Selleri, IL Weissman, LA Herzenberg, ML Cleary
Blood, 2007ashpublications.org
Pbx1, a homeodomain transcription factor that was originally identified as the product of a
proto-oncogene in acute pre-B–cell leukemia, is a global regulator of embryonic
development. However, embryonic lethality in its absence has prevented an assessment of
its role in B-cell development. Here, using Rag1-deficient blastocyst complementation
assays, we demonstrate that Pbx1 null embryonic stem (ES) cells fail to generate common
lymphoid progenitors (CLPs) resulting in a complete lack of B and NK cells, and a partial …
Abstract
Pbx1, a homeodomain transcription factor that was originally identified as the product of a proto-oncogene in acute pre-B–cell leukemia, is a global regulator of embryonic development. However, embryonic lethality in its absence has prevented an assessment of its role in B-cell development. Here, using Rag1-deficient blastocyst complementation assays, we demonstrate that Pbx1 null embryonic stem (ES) cells fail to generate common lymphoid progenitors (CLPs) resulting in a complete lack of B and NK cells, and a partial impairment of T-cell development in chimeric mice. A critical role for Pbx1 was confirmed by rescue of B-cell development from CLPs following restoration of its expression in Pbx1-deficient ES cells. In adoptive transfer experiments, B-cell development from Pbx1-deficient fetal liver cells was also severely compromised, but not erased, since transient B lymphopoiesis was detected in Rag-deficient recipients. Conditional inactivation of Pbx1 in pro-B (CD19+) cells and thereafter revealed that Pbx1 is not necessary for B-cell development to proceed from the pro-B–cell stage. Thus, Pbx1 critically functions at a stage between hematopoietic stem cell development and B-cell commitment and, therefore, is one of the earliest-acting transcription factors that regulate de novo B-lineage lymphopoiesis.
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