AI Article Synopsis
- B lymphocytes are formed from stem cells through a series of steps regulated by transcription factors, notably early B cell factor (EBF).
- EBF is crucial for the decision-making process of progenitor cells to become B cells, as its absence prevents the expression of key B cell markers.
- EBF activates important genes, including Pax5, which together enhance the commitment of cells to the B cell lineage—highlighting EBF's central role in B cell development.
Article Abstract
B lymphocytes are generated from hematopoietic stem cells in a series of steps controlled by transcription factors. One of the most important regulators of this process is early B cell factor (EBF). Multiple lines of evidence indicate that expression of EBF is a principle determinant of the B cell fate. In the absence of EBF, progenitor cells fail to express classical markers of B cells, including immunoglobulins. EBF drives B cell differentiation by activating the Pax5 gene and other genes required for the pre-B and B cell receptors. New evidence suggests that expression of EBF in common lymphoid progenitors directs B cell fate decisions. Specification and commitment of cells to the B cell lineage are further established by Pax5, which increases expression of EBF. Recently, it was demonstrated that both EBF and Pax5 contribute to the commitment of cells to the B lineage. Together, these studies confirm that EBF is a keystone in the regulatory network that coordinates B cell lineage specification and commitment.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2577021 | PMC |
| http://dx.doi.org/10.1016/j.smim.2008.07.004 | DOI Listing |
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