Promoters, enhancers, and transcription target RAG1 binding during V(D)J recombination

Ji, Yanhong; Little, Alicia J.; Banerjee, Joydeep K.; Hao, Bingtao; Oltz, Eugene M.; Krangel, Michael S.; Schatz, David G.

doi:10.1084/jem.20101136

Cited by 67 publications

(62 citation statements)

References 30 publications

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“…The second step would be the generation of accessibility at the recombination signal sequences (RSSs), which is likely to be accomplished by transcription through the V, D, or J genes and the RSS, which also endows the gene with H3K4me3 and thus will aid in RAG2 recruitment (30,31). Furthermore, RAG1 binding is dependent upon intact promoters and enhancers as well as on transcription across the RSS (37).…”

Section: Discussionmentioning

confidence: 99%

Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Verma-Gaur

Torkamani

Schaffer

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

102

122

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Noncoding sense and antisense germ-line transcription within the Ig heavy chain locus precedes V(D)J recombination and has been proposed to be associated with Igh locus accessibility, although its precise role remains elusive. However, no global analysis of germline transcription throughout the Igh locus has been done. Therefore, we performed directional RNA-seq, demonstrating the locations and extent of both sense and antisense transcription throughout the Igh locus. Surprisingly, the majority of antisense transcripts are localized around two Pax5-activated intergenic repeat (PAIR) elements in the distal IghV region. Importantly, long-distance loops measured by chromosome conformation capture (3C) are observed between these two active PAIR promoters and Eμ, the start site of Iμ germ-line transcription, in a lineage-and stage-specific manner, even though this antisense transcription is Eμ-independent. YY1 −/− pro-B cells are greatly impaired in distal V H gene rearrangement and Igh locus compaction, and we demonstrate that YY1 deficiency greatly reduces antisense transcription and PAIR-Eμ interactions. ChIP-seq shows high level YY1 binding only at Eμ, but low levels near some antisense promoters. PAIR-Eμ interactions are not disrupted by DRB, which blocks transcription elongation without disrupting transcription factories once they are established, but the looping is reduced after heat-shock treatment, which disrupts transcription factories. We propose that transcription-mediated interactions, most likely at transcription factories, initially compact the Igh locus, bringing distal V H genes close to the DJ H rearrangement which is adjacent to Eμ. Therefore, we hypothesize that one key role of noncoding germ-line transcription is to facilitate locus compaction, allowing distal V H genes to undergo efficient rearrangement.A ntigen receptors in lymphocytes are assembled in the highly regulated lineage-specific process of V(D)J recombination, which creates a diverse repertoire of Ig and T-cell receptors. In each precursor lymphocyte, one each of the many V, D, and J gene segments at the appropriate receptor loci are juxtaposed to create a V(D)J exon encoding the variable region of the antigen receptor. In B-lineage progenitors, rearrangement occurs first at the Ig heavy chain (Igh) locus, where D H to J H rearrangement occurs first on both alleles, followed by V H to DJ H rearrangement (1). After successful rearrangement of the Igh locus, rearrangement at the Igk light chain locus begins. These successive stages of rearrangement have been proposed to be regulated by differential accessibility of different portions of the loci at the appropriate time for rearrangement (2). Early indications of this stage-specific and lineage-specific accessibility came from the observation that unrearranged gene segments underwent noncoding transcription at the stage immediately preceding their rearrangement (3, 4).The murine Igh locus spans ∼2.8 Mb, of which ∼2.4 Mb contains the 195 V H gene segments (5). The V H genes are divided i...

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Section: Discussionmentioning

confidence: 99%

Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Verma-Gaur

Torkamani

Schaffer

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

102

122

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“…Subsequently, this model has been strengthened by findings that link V(D)J recombination to transcriptional control elements, such as AR-associated enhancers and promoters, and to several molecular parameters related to open chromatin (including association with active histone marks, DNA hypomethylation, and nuclease hypersensitivity) (3,5). Robust germline transcription at *Centre d'Immunologie de Marseille-Luminy, Aix-Marseille University, UM2, 13288 Marseille, France; (D)J clusters is an initial activation event at all AR loci that generates a focal zone of RAG1/2 binding, termed the recombination center (6,7). More insight into the accessibility model was provided by recent studies demonstrating that the PHD finger domain of RAG2 binds with high affinity to histone H3 trimethylated at K4 (H3K4me3) and that RAG2 is recruited to H3K4me3 domains genome-wide (6)(7)(8).…”

mentioning

confidence: 99%

“…Robust germline transcription at *Centre d'Immunologie de Marseille-Luminy, Aix-Marseille University, UM2, 13288 Marseille, France; (D)J clusters is an initial activation event at all AR loci that generates a focal zone of RAG1/2 binding, termed the recombination center (6,7). More insight into the accessibility model was provided by recent studies demonstrating that the PHD finger domain of RAG2 binds with high affinity to histone H3 trimethylated at K4 (H3K4me3) and that RAG2 is recruited to H3K4me3 domains genome-wide (6)(7)(8).…”

mentioning

confidence: 99%

Transcription-Dependent Generation of a Specialized Chromatin Structure at the TCRβ Locus

Zacarías-Cabeza

Belhocine

Vanhille

et al. 2015

The Journal of Immunology

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“…It is well known that chromatin organization influences the ability of RAG to gain access to an authentic RSS. 75 Therefore, access to a cRSS is also decisive for the occurrence of RAG-cRSS mistargeted DSB induction at oncogene loci sites. Reactivity of the RAG protein complex is not only dependent on the recognition of a cRSS by RAG1, but it is likewise dependent on the ability of RAG2 to bind to a H3K4me3-modified nucleosome adjacent to that cRSS in order to enable cleavage at that cRSS site.…”

Section: The Role Of the V(d)j Recombination Machinery In Dsb Inductimentioning

confidence: 99%

Breakpoint sites disclose the role of the V(D)J recombination machinery in the formation of T-cell receptor (TCR) and non-TCR associated aberrations in T-cell acute lymphoblastic leukemia

et al. 2013

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Aberrant recombination between T-cell receptor genes and oncogenes gives rise to chromosomal translocations that are genetic hallmarks in several subsets of human T-cell acute lymphoblastic leukemias. The V(D)J recombination machinery has been shown to play a role in the formation of these T-cell receptor translocations. Other, non-T-cell receptor chromosomal aberrations, such as SIL-TAL1 deletions, have likewise been recognized as V(D)J recombination associated aberrations. Despite the postulated role of V(D)J recombination, the extent of the V(D)J recombination machinery involvement in the formation of T-cell receptor and non-T-cell receptor aberrations in T-cell acute lymphoblastic leukemia is still poorly understood. We performed a comprehensive in silico and ex vivo evaluation of 117 breakpoint sites from 22 different T-cell receptor translocation partners as well as 118 breakpoint sites from non-T-cell receptor chromosomal aberrations. Based on this extensive set of breakpoint data, we provide a comprehensive overview of T-cell receptor and oncogene involvement in T-ALL. Moreover, we assessed the role of the V(D)J recombination machinery in the formation of chromosomal aberrations, and propose an up-dated mechanistic classification on how the V(D)J recombination machinery contributes to the formation of T-cell receptor and non-T-cell receptor aberrations in human T-cell acute lymphoblastic leukemia.

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Promoters, enhancers, and transcription target RAG1 binding during V(D)J recombination

Abstract: RAG1 binding to TCR gene elements is dictated by transcriptional control elements and by transcription itself; these findings provide direct confirmation of the long-held accessibility model.

Cited by 67 publications

References 30 publications

Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Transcription-Dependent Generation of a Specialized Chromatin Structure at the TCRβ Locus

Breakpoint sites disclose the role of the V(D)J recombination machinery in the formation of T-cell receptor (TCR) and non-TCR associated aberrations in T-cell acute lymphoblastic leukemia

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Promoters, enhancers, and transcription target RAG1 binding during V(D)J recombination

Abstract: RAG1 binding to TCR gene elements is dictated by transcriptional control elements and by transcription itself; these findings provide direct confirmation of the long-held accessibility model.

Cited by 67 publications

References 30 publications

Noncoding transcription within the Igh distal V H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Noncoding transcription within the Igh distal V H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Transcription-Dependent Generation of a Specialized Chromatin Structure at the TCRβ Locus

Breakpoint sites disclose the role of the V(D)J recombination machinery in the formation of T-cell receptor (TCR) and non-TCR associated aberrations in T-cell acute lymphoblastic leukemia

Contact Info

Product

Resources

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Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells

Noncoding transcription within the Igh distal V _H region at PAIR elements affects the 3D structure of the Igh locus in pro-B cells