Regulation of TCR {delta} and {alpha} repertoires by local and long-distance control of variable gene segment chromatin structure

doi:10.1084/jem.20050680

Published online 8 August 2005 doi:10.1084/jem.20050680
Rockefeller University Press, 0022-1007 $8.00
JEM, Volume 202, Number 4, 467-472

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BRIEF DEFINITIVE REPORT

Regulation of TCR ${delta}$ and ${alpha}$ repertoires by local and long-distance control of variable gene segment chromatin structure

Abbas Hawwari and Michael S. Krangel

Department of Immunology, Duke University Medical Center, Durham, NC 27710

CORRESPONDENCE Michael S. Krangel: krang001{at}mc.duke.edu

Murine Tcrd and Tcra gene segments reside in a single geneticlocus and undergo recombination in CD4^–CD8^– (doublenegative [DN]) and CD4⁺CD8⁺ (double positive [DP]) thymocytes,respectively. TcraTcrd locus variable gene segments are subjectto complex regulation. Only a small subset of $~$ 100 variable genesegments contributes substantially to the adult TCR ${delta}$ repertoire.Moreover, although most contribute to the TCR ${alpha}$ repertoire, variablegene segments that are J ${alpha}$ proximal are preferentially used duringprimary Tcra recombination. We investigate the role of localchromatin accessibility in determining the developmental patternof TcraTcrd locus variable gene segment recombination. We findvariable gene segments to be heterogeneous with respect to acetylationof histones H3 and H4. Those that dominate the adult TCR ${delta}$ repertoireare hyperacetylated in DN thymocytes, independent of their positionin the locus. Moreover, proximal variable gene segments showdramatic increases in histone acetylation and germline transcriptionin DP thymocytes, a result of super long-distance regulationby the Tcra enhancer. Our results imply that differences inchromatin accessibility contribute to biases in TcraTcrd locusvariable gene segment recombination in DN and DP thymocytesand extend the distance over which the Tcra enhancer can regulatechromatin structure to a remarkable 525 kb.

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