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Blood, 15 September 2004, Vol. 104, No. 6, pp. 1593.
A mastermind revealedMASSACHUSETTS GENERAL HOSPITAL AND HARVARD MEDICAL SCHOOL
Retroviral transduction of hematopoietic stem cells with a dominant interfering form of Mastermind has revealed an in vivo role in vertebrates for the Mastermind-like family of Notch regulators during lymphocyte development.
In hematopoietic cells in vertebrates, the Notch pathway appears to serve as a means to ensure that selected lineage commitment events proceed in a binary manner. In central lymphoid organs such as the bone marrow and thymus, the decision to become a T cell rather than a B cell requires signaling via Notch1. Two distinct B-lymphocyte lineages develop in the spleen. Mature follicular B lymphocytes are recirculating cells that mature in response to antigen receptor-derived signals. A second lineage of B cells, known as marginal zone (MZ) B cells, resides in close proximity to specialized macrophages that surround an anastomosing arteriolar sinus known as the marginal sinus. MZ B cells are extremely long-lived lymphocytes that respond rapidly to blood-borne pathogens and can participate in both T-independent as well as T-dependent immune responses. These B cells do not develop from clones that receive relatively strong antigen receptor-mediated signals1 but require signals from Notch2 and its ligand delta-like-1,2-4 as revealed by conditional gene targeting studies. Notch2 apparently intercedes during B-cell development to ensure the generation of a second B-cell lineage in the spleen. Maillard and colleagues report the transduction of lymphoid progenitors with a truncated N-terminal form of Mastermind-like-1 (MAML1) that can associate with intracellular Notch but lacks the C-terminal transcriptional activation domain of the full-length protein. This dominant interfering MAML1 blocks Notch1-dependent T-lineage commitment and Notch2-dependent MZ B-cell development, thus demonstrating an in vivo function for Mastermind in vertebrates. Expression in lymphoid progenitors of wild-type Deltex1 blocks commitment to the T-lineage but does not block MZ B-cell development. It is possible that Deltex 1 might actually function as a negative regulator of Notch1 in the bone marrow and a positive regulator of Notch2 signaling in the spleen. There are 3 Mastermind-like genes in vertebrates, and conditional inactivation of MAML1, MAML2, and MAML3 may be required to elucidate which Mastermind ortholog(s) regulates Notch transcription during lymphocyte development in the bone marrow and the spleen. References
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| Copyright © 2004 by American Society of Hematology Online ISSN: 1528-0020 | |||||||||
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