TCRβ Feedback Signals Inhibit the Coupling of Recombinationally Accessible Vβ14 Segments with DJβ Complexes

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Jaenisch, RudolfYang-Iott, Katherine S.Carpenter, Andrea C.Rowh, Marta A. W.Steinel, Natalie; ... Show more
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Abstract
Ag receptor allelic exclusion is thought to occur through monoallelic initiation and subsequent feedback inhibition of recombinational accessibility. However, our previous analysis of mice containing a V(D)J recombination reporter inserted into Vβ14 (Vβ14[superscript Rep]) indicated that Vβ14 chromatin accessibility is biallelic. To determine whether Vβ14 recombinational accessibility is subject to feedback inhibition, we analyzed TCRβ rearrangements in Vβ14[superscript Rep] mice containing a preassembled in-frame transgenic Vβ8.2Dβ1Jβ1.1 or an endogenous Vβ14Dβ1Jβ1.4 rearrangement on the homologous chromosome. Expression of either preassembled VβDJβC β-chain accelerated thymocyte development because of enhanced cellular selection, demonstrating that the rate-limiting step in early αβ T cell development is the assembly of an in-frame VβDJβ rearrangement. Expression of these preassembled VβDJβ rearrangements inhibited endogenous Vβ14-to-DJβ rearrangements as expected. However, in contrast to results predicted by the accepted model of TCRβ feedback inhibition, we found that expression of these preassembled TCR β-chains did not downregulate recombinational accessibility of Vβ14 chromatin. Our findings suggest that TCRβ-mediated feedback inhibition of Vβ14 rearrangements depends on inherent properties of Vβ14, Dβ, and Jβ recombination signal sequences.
Date issued
2009-12
URI
http://hdl.handle.net/1721.1/73894
Department
Massachusetts Institute of Technology. Department of BiologyWhitehead Institute for Biomedical Research
Journal
Journal of Immunology
Publisher
American Association of Immunologists
Citation
Yang-Iott, K. S. et al. “TCR  Feedback Signals Inhibit the Coupling of Recombinationally Accessible V 14 Segments with DJ  Complexes.” The Journal of Immunology 184.3 (2009): 1369–1378.
Version: Author's final manuscript
ISSN
0022-1767
1550-6606
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