Literature DB >> 26101321

Domain-Specific and Stage-Intrinsic Changes in Tcrb Conformation during Thymocyte Development.

Kinjal Majumder1, Levi J Rupp2, Katherine S Yang-Iott2, Olivia I Koues1, Katherine E Kyle1, Craig H Bassing3, Eugene M Oltz4.   

Abstract

Considerable cross-talk exists between mechanisms controlling genome architecture and gene expression. AgR loci are excellent models for these processes because they are regulated at both conformational and transcriptional levels to facilitate their assembly by V(D)J recombination. Upon commitment to the double-negative stage of T cell development, Tcrb adopts a compact conformation that promotes long-range recombination between Vβ gene segments (Trbvs) and their DβJβ targets. Formation of a functional VβDβJβ join signals for robust proliferation of double-negative thymocytes and their differentiation into double-positive (DP) cells, where Trbv recombination is squelched (allelic exclusion). DP differentiation also is accompanied by decontraction of Tcrb, which has been thought to separate the entire Trbv cluster from DβJβ segments (spatial segregation-based model for allelic exclusion). However, DP cells also repress transcription of unrearranged Trbvs, which may contribute to allelic exclusion. We performed a more detailed study of developmental changes in Tcrb topology and found that only the most distal portion of the Trbv cluster separates from DβJβ segments in DP thymocytes, leaving most Trbvs spatially available for rearrangement. Preferential dissociation of distal Trbvs is independent of robust proliferation or changes in transcription, chromatin, or architectural factors, which are coordinately regulated across the entire Trbv cluster. Segregation of distal Trbvs also occurs on alleles harboring a functional VβDβJβ join, suggesting that this process is independent of rearrangement status and is DP intrinsic. Our finding that most Trbvs remain associated with DβJβ targets in DP cells revises allelic exclusion models from their current conformation-dominant to a transcription-dominant formulation.
Copyright © 2015 by The American Association of Immunologists, Inc.

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Year:  2015        PMID: 26101321      PMCID: PMC4506872          DOI: 10.4049/jimmunol.1500692

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  52 in total

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Review 2.  Accessibility control of V(D)J recombination.

Authors:  Robin Milley Cobb; Kenneth J Oestreich; Oleg A Osipovich; Eugene M Oltz
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3.  Reversible contraction by looping of the Tcra and Tcrb loci in rearranging thymocytes.

Authors:  Jane A Skok; Ramiro Gisler; Maria Novatchkova; Deborah Farmer; Wouter de Laat; Meinrad Busslinger
Journal:  Nat Immunol       Date:  2007-03-04       Impact factor: 25.606

4.  A plant homeodomain in RAG-2 that binds Hypermethylated lysine 4 of histone H3 is necessary for efficient antigen-receptor-gene rearrangement.

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5.  Early TCR expression and aberrant T cell development in mice with endogenous prerearranged T cell receptor genes.

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Authors:  Tae Hoon Kim; Ziedulla K Abdullaev; Andrew D Smith; Keith A Ching; Dmitri I Loukinov; Roland D Green; Michael Q Zhang; Victor V Lobanenkov; Bing Ren
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10.  Regulation of Vbeta germline transcription in RAG-deficient mice by the CD3epsilon-mediated signals: implication of Vbeta transcriptional regulation in TCR beta allelic exclusion.

Authors:  M Senoo; Y Shinkai
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Authors:  Yue Huang; Olivia I Koues; Jiang-Yang Zhao; Regina Liu; Sarah C Pyfrom; Jacqueline E Payton; Eugene M Oltz
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3.  DNA double-strand breaks induce H2Ax phosphorylation domains in a contact-dependent manner.

Authors:  Patrick L Collins; Caitlin Purman; Sofia I Porter; Vincent Nganga; Ankita Saini; Katharina E Hayer; Greer L Gurewitz; Barry P Sleckman; Jeffrey J Bednarski; Craig H Bassing; Eugene M Oltz
Journal:  Nat Commun       Date:  2020-06-22       Impact factor: 14.919

Review 4.  Regulation of T-cell Receptor Gene Expression by Three-Dimensional Locus Conformation and Enhancer Function.

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Review 5.  Transcriptional Regulation of Early T-Lymphocyte Development in Thymus.

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Journal:  Front Immunol       Date:  2022-03-31       Impact factor: 7.561

6.  RSSs set the odds for exclusion.

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  6 in total

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