Literature DB >> 21844384

Differential regulation of proximal and distal Vbeta segments upstream of a functional VDJbeta1 rearrangement upon beta-selection.

Brenna L Brady1, Craig H Bassing.   

Abstract

Developmental stage-specific regulation of transcriptional accessibility helps control V(D)J recombination. Vβ segments on unrearranged TCRβ alleles are accessible in CD4(-)/CD8(-) (double-negative [DN]) thymocytes, when they recombine, and inaccessible in CD4(+)/CD8(+) (double-positive [DP]) thymocytes, when they do not rearrange. Downregulation of Vβ accessibility on unrearranged alleles is linked with Lat-dependent β-selection signals that inhibit Vβ rearrangement, stimulate Ccnd3-driven proliferation, and promote DN-to-DP differentiation. Transcription and recombination of Vβs on VDJβ-rearranged alleles in DN cells has not been studied; Vβs upstream of functional VDJβ rearrangements have been found to remain accessible, yet not recombine, in DP cells. To elucidate contributions of β-selection signals in regulating Vβ transcription and recombination on VDJβ-rearranged alleles, we analyzed wild-type, Ccnd3(-/-), and Lat(-/-) mice containing a preassembled functional Vβ1DJCβ1 (Vβ1(NT)) gene. Vβ10 segments located just upstream of this VDJCβ1 gene were the predominant germline Vβs that rearranged in Vβ1(NT/NT) and Vβ1(NT/NT)Ccnd3(-/-) thymocytes, whereas Vβ4 and Vβ16 segments located further upstream rearranged at similar levels as Vβ10 in Vβ1(NT/NT)Lat(-/-) DN cells. We previously showed that Vβ4 and Vβ16, but not Vβ10, are transcribed on Vβ1(NT) alleles in DP thymocytes; we now demonstrate that Vβ4, Vβ16, and Vβ10 are transcribed at similar levels in Vβ1(NT/NT)Lat(-/-) DN cells. These observations indicate that suppression of Vβ rearrangements is not dependent on Ccnd3-driven proliferation, and DN residence can influence the repertoire of Vβs that recombine on alleles containing an assembled VDJCβ1 gene. Our findings also reveal that β-selection can differentially silence rearrangement of germline Vβ segments located proximal and distal to functional VDJβ genes.

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Year:  2011        PMID: 21844384      PMCID: PMC3169729          DOI: 10.4049/jimmunol.1101079

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


  44 in total

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2.  Essential role of LAT in T cell development.

Authors:  W Zhang; C L Sommers; D N Burshtyn; C C Stebbins; J B DeJarnette; R P Trible; A Grinberg; H C Tsay; H M Jacobs; C M Kessler; E O Long; P E Love; L E Samelson
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7.  Transcription and demethylation of TCR beta gene initiate prior to the gene rearrangement in c-kit+ thymocytes with CD3 expression: evidence of T cell commitment in the thymus.

Authors:  K Hozumi; A Kobori; T Sato; T Nishimura; S Habu
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8.  Regulation of Vbeta germline transcription in RAG-deficient mice by the CD3epsilon-mediated signals: implication of Vbeta transcriptional regulation in TCR beta allelic exclusion.

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9.  Productive T-cell receptor beta-chain gene rearrangement: coincident regulation of cell cycle and clonality during development in vivo.

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Journal:  Genes Dev       Date:  1996-04-15       Impact factor: 11.361

10.  The timing of TCR alpha expression critically influences T cell development and selection.

Authors:  Troy A Baldwin; Michelle M Sandau; Stephen C Jameson; Kristin A Hogquist
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2.  Noncore RAG1 regions promote Vβ rearrangements and αβ T cell development by overcoming inherent inefficiency of Vβ recombination signal sequences.

Authors:  Julie E Horowitz; Craig H Bassing
Journal:  J Immunol       Date:  2014-01-10       Impact factor: 5.422

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

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Journal:  J Immunol       Date:  2015-06-22       Impact factor: 5.422

4.  Requirement for dicer in survival of proliferating thymocytes experiencing DNA double-strand breaks.

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Journal:  J Immunol       Date:  2013-02-20       Impact factor: 5.422

Review 5.  Placing ion channels into a signaling network of T cells: from maturing thymocytes to healthy T lymphocytes or leukemic T lymphoblasts.

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Journal:  Biomed Res Int       Date:  2015-03-19       Impact factor: 3.411

6.  Allelic exclusion of the immunoglobulin heavy chain locus is independent of its nuclear localization in mature B cells.

Authors:  Sjoerd J B Holwerda; Harmen J G van de Werken; Claudia Ribeiro de Almeida; Ingrid M Bergen; Marjolein J W de Bruijn; Marjon J A M Verstegen; Marieke Simonis; Erik Splinter; Patrick J Wijchers; Rudi W Hendriks; Wouter de Laat
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  6 in total

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