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Publication : Redundant and nonredundant functions of ATM and H2AX in αβ T-lineage lymphocytes.

First Author  Yin B Year  2012
Journal  J Immunol Volume  189
Issue  3 Pages  1372-9
PubMed ID  22730535 Mgi Jnum  J:189790
Mgi Id  MGI:5446996 Doi  10.4049/jimmunol.1200829
Citation  Yin B, et al. (2012) Redundant and nonredundant functions of ATM and H2AX in alphabeta T-lineage lymphocytes. J Immunol 189(3):1372-9
abstractText  The ataxia telangiectasia mutated (ATM) kinase and H2AX histone tumor suppressor proteins are each critical for maintenance of cellular genomic stability and suppression of lymphomas harboring clonal translocations. ATM is the predominant kinase that phosphorylates H2AX in chromatin around DNA double-strand breaks, including along lymphocyte Ag receptor loci cleaved during V(D)J recombination. However, combined germline inactivation of Atm and H2ax in mice causes early embryonic lethality associated with substantial cellular genomic instability, indicating that ATM and H2AX exhibit nonredundant functions in embryonic cells. To evaluate potential nonredundant roles of ATM and H2AX in somatic cells, we generated and analyzed Atm-deficient mice with conditional deletion of H2ax in alphabeta T-lineage lymphocytes. Combined Atm/H2ax inactivation starting in early-stage CD4(-)/CD8(-) thymocytes resulted in lower numbers of later-stage CD4(+)/CD8(+) thymocytes, but led to no discernible V(D)J recombination defect in G1 phase cells beyond that observed in Atm-deficient cells. H2ax deletion in Atm-deficient thymocytes also did not affect the incidence or mortality of mice from thymic lymphomas with clonal chromosome 14 (TCRalpha/delta) translocations. Yet, in vitro-stimulated Atm/H2ax-deficient splenic alphabeta T cells exhibited a higher frequency of genomic instability, including radial chromosome translocations and TCRbeta translocations, compared with cells lacking Atm or H2ax. Collectively, our data demonstrate that both redundant and nonredundant functions of ATM and H2AX are required for normal recombination of TCR loci, proliferative expansion of developing thymocytes, and maintenance of genomic stability in cycling alphabeta T-lineage cells.
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