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Publication : ISWI ATPase Smarca5 Regulates Differentiation of Thymocytes Undergoing β-Selection.

First Author  Zikmund T Year  2019
Journal  J Immunol Volume  202
Issue  12 Pages  3434-3446
PubMed ID  31068388 Mgi Jnum  J:275887
Mgi Id  MGI:6307186 Doi  10.4049/jimmunol.1801684
Citation  Zikmund T, et al. (2019) ISWI ATPase Smarca5 Regulates Differentiation of Thymocytes Undergoing beta-Selection. J Immunol 202(12):3434-3446
abstractText  Development of lymphoid progenitors requires a coordinated regulation of gene expression, DNA replication, and gene rearrangement. Chromatin-remodeling activities directed by SWI/SNF2 superfamily complexes play important roles in these processes. In this study, we used a conditional knockout mouse model to investigate the role of Smarca5, a member of the ISWI subfamily of such complexes, in early lymphocyte development. Smarca5 deficiency results in a developmental block at the DN3 stage of alphabeta thymocytes and pro-B stage of early B cells at which the rearrangement of Ag receptor loci occurs. It also disturbs the development of committed (CD73(+)) gammadelta thymocytes. The alphabeta thymocyte block is accompanied by massive apoptotic depletion of beta-selected double-negative DN3 cells and premitotic arrest of CD4/CD8 double-positive cells. Although Smarca5-deficient alphabeta T cell precursors that survived apoptosis were able to undergo a successful TCRbeta rearrangement, they exhibited a highly abnormal mRNA profile, including the persistent expression of CD44 and CD25 markers characteristic of immature cells. We also observed that the p53 pathway became activated in these cells and that a deficiency of p53 partially rescued the defect in thymus cellularity (in contrast to early B cells) of Smarca5-deficient mice. However, the activation of p53 was not primarily responsible for the thymocyte developmental defects observed in the Smarca5 mutants. Our results indicate that Smarca5 plays a key role in the development of thymocytes undergoing beta-selection, gammadelta thymocytes, and also B cell progenitors by regulating the transcription of early differentiation programs.
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