Chromatin Domain Organization of the TCRb Locus and Its Perturbation by Ectopic CTCF Binding

Rawat, Pratishtha; Jalan, Manisha; Sadhu, Ananya; Kanaujia, Abhilasha; Srivastava, M. P.

doi:10.1128/mcb.00557-16

Cited by 13 publications

(13 citation statements)

References 53 publications

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“…However, it is unclear whether new loops can be established between endogenous and ectopically inserted CTCF sites. Early 3C observations suggested that ectopic sequences containing CTCF sites can change the surrounding chromosomal interactions39,40; however, experimental resolution in 3C did not allow to resolve single CTCF loops, and inserted sequences contained additional regulatory regions. Since piggyBac-TetO constructs alone do not perturb chromosome structure, we further engineered them to insert ectopic CTCF sites in the genome and detect resulting structural modifications without confounding effects.…”

Section: Resultsmentioning

confidence: 99%

DamC reveals principles of chromatin folding in vivo without crosslinking and ligation

Redolfi

Zhan

Valdes-Quezada

et al. 2019

Nat Struct Mol Biol

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Current understanding of chromosome folding largely relies on chromosome conformation capture (3C)-based experiments, where chromosomal interactions are detected as ligation products after chromatin crosslinking. To measure chromosome structure in vivo , quantitatively and without crosslinking and ligation, we implemented a modified version of DamID named DamC, which combines DNA-methylation based detection of chromosomal interactions with next-generation sequencing and biophysical modelling of methylation kinetics. DamC performed in mouse embryonic stem cells provides the first in vivo validation of the existence of topologically associating domains (TADs), CTCF loops and confirms 3C-based measurements of the scaling of contact probabilities. Combining DamC with transposon-mediated genomic engineering shows that new loops can be formed between ectopic and endogenous CTCF sites, which redistributes physical interactions within TADs. DamC provides the first crosslinking- and ligation-free demonstration of the existence of key structural features of chromosomes and provides novel insights into how chromosome structure within TADs can be manipulated.

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Section: Resultsmentioning

confidence: 99%

DamC reveals principles of chromatin folding in vivo without crosslinking and ligation

Redolfi

Zhan

Valdes-Quezada

et al. 2019

Nat Struct Mol Biol

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“…Also, in the TCRβ locus, the CTCF site near Eβ has been reported to interact very strongly with the poorly occupied CTCF site just upstream of the promoter of Dβ1, PDβ1, even though those CTCF sites are in tandem orientation. However, the CTCF site near PDβ1 is in the same HindIII fragment as PDβ1, so it is not clear if those 3C experiments are reveal CTCF–CTCF interactions or CTCF interactions with the PDβ1 promoter itself ( 81 ). We have previously documented that Eμ is recruited to the interacting CTCF sites at IGCR1 and 3′RR, and the same could be happening here ( 36 ).…”

Section: Discussionmentioning

confidence: 99%

Variable Extent of Lineage-Specificity and Developmental Stage-Specificity of Cohesin and CCCTC-Binding Factor Binding Within the Immunoglobulin and T Cell Receptor Loci

et al. 2018

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CCCTC-binding factor (CTCF) is largely responsible for the 3D architecture of the genome, in concert with the action of cohesin, through the creation of long-range chromatin loops. Cohesin is hypothesized to be the main driver of these long-range chromatin interactions by the process of loop extrusion. Here, we performed ChIP-seq for CTCF and cohesin in two stages each of T and B cell differentiation and examined the binding pattern in all six antigen receptor (AgR) loci in these lymphocyte progenitors and in mature T and B cells, ES cells, and fibroblasts. The four large AgR loci have many bound CTCF sites, most of which are only occupied in lymphocytes, while only the CTCF sites at the end of each locus near the enhancers or J genes tend to be bound in non-lymphoid cells also. However, despite the generalized lymphocyte restriction of CTCF binding in AgR loci, the Igκ locus is the only locus that also shows significant lineage-specificity (T vs. B cells) and developmental stage-specificity (pre-B vs. pro-B) in CTCF binding. We show that cohesin binding shows greater lineage- and stage-specificity than CTCF at most AgR loci, providing more specificity to the loops. We also show that the culture of pro-B cells in IL7, a common practice to expand the number of cells before ChIP-seq, results in a CTCF-binding pattern resembling pre-B cells, as well as other epigenetic and transcriptional characteristics of pre-B cells. Analysis of the orientation of the CTCF sites show that all sites within the large V portions of the Igh and TCRβ loci have the same orientation. This suggests either a lack of requirement for convergent CTCF sites creating loops, or indicates an absence of any loops between CTCF sites within the V region portion of those loci but only loops to the convergent sites at the D-J-enhancer end of each locus. The V region portions of the Igκ and TCRα/δ loci, by contrast, have CTCF sites in both orientations, providing many options for creating CTCF-mediated convergent loops throughout the loci. CTCF/cohesin loops, along with transcription factors, drives contraction of AgR loci to facilitate the creation of a diverse repertoire of antibodies and T cell receptors.

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“…Similar to the architectural changes observed at the TCRα/TCRδ locus during thymocyte development [ 50 ], distinct genomic conformations have been observed by confocal microscopy at the TCRβ locus during DN3a to DP differentiation [ 51 ] ( Figure 6 b). In DN3a thymocytes, the entire TCRβ locus presents a completely compacted configuration, bringing all Vβ gene segments into spatial proximity to the 25-kb TCRβ D-J region to assure a diverse TCRβ repertoire [ 51 , 59 , 60 , 61 , 62 , 63 ]. This locus architecture is thought to be mediated by CTCF/cohesin binding to CBSs associated with half of the Vβ gene segments (such as the A, B, and C sites), two intergenic sites located upstream of the Dβ gene segments (5′PC and D sites), and another one (E site) located downstream of the TCRβ enhancer (Eβ).…”

Section: Architectural Changes At the Tcr Regions During Thymocytementioning

confidence: 99%

“…This locus architecture is thought to be mediated by CTCF/cohesin binding to CBSs associated with half of the Vβ gene segments (such as the A, B, and C sites), two intergenic sites located upstream of the Dβ gene segments (5′PC and D sites), and another one (E site) located downstream of the TCRβ enhancer (Eβ). CBSs associated to the Vβ gene segments are all oriented convergently toward the 5′PC, D, and E sites [ 47 , 63 ], allowing CTCF-CTCF looping formation. These loops bring the Vβ gene segments into the vicinity of the DβJβ region via locus contraction.…”

Section: Architectural Changes At the Tcr Regions During Thymocytementioning

confidence: 99%

“…The TCRβ RC is defined by Eβ-Dβ1 promoter and Eβ-Dβ2 promoter loops formed in a 25-kb region [ 61 , 72 ], emphasizing Eβ as the crucial element in RC establishment ( Figure 6 b). In contrast with the TCRδ and TCRα RCs, where CTCF and cohesin bind to convergent CBSs and play a functional role in RC formation [ 52 , 53 , 71 ], no convergently oriented CBSs are found within the TCRβ RC (5′PC, D, and E sites have the same orientation) [ 47 , 63 ]. However, tandem CBSs flanking the TCRβ RC can create coiled loops that could contribute to the formation and stabilization of this RC as well as to the configuration of specific loops that facilitate RSS synapsis and recombination.…”

Section: Architectural Changes At the Tcr Regions During Thymocytementioning

confidence: 99%

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

Rodríguez-Caparrós

Álvarez-Santiago

Valle-Pastor

et al. 2020

IJMS

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The adaptive immune response in vertebrates depends on the expression of antigen-specific receptors in lymphocytes. T-cell receptor (TCR) gene expression is exquisitely regulated during thymocyte development to drive the generation of αβ and γδ T lymphocytes. The TCRα, TCRβ, TCRγ, and TCRδ genes exist in two different configurations, unrearranged and rearranged. A correctly rearranged configuration is required for expression of a functional TCR chain. TCRs can take the form of one of three possible heterodimers, pre-TCR, TCRαβ, or TCRγδ which drive thymocyte maturation into αβ or γδ T lymphocytes. To pass from an unrearranged to a rearranged configuration, global and local three dimensional (3D) chromatin changes must occur during thymocyte development to regulate gene segment accessibility for V(D)J recombination. During this process, enhancers play a critical role by modifying the chromatin conformation and triggering noncoding germline transcription that promotes the recruitment of the recombination machinery. The different signaling that thymocytes receive during their development controls enhancer activity. Here, we summarize the dynamics of long-distance interactions established through chromatin regulatory elements that drive transcription and V(D)J recombination and how different signaling pathways are orchestrated to regulate the activity of enhancers to precisely control TCR gene expression during T-cell maturation.

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Chromatin Domain Organization of the TCRb Locus and Its Perturbation by Ectopic CTCF Binding

Cited by 13 publications

References 53 publications

DamC reveals principles of chromatin folding in vivo without crosslinking and ligation

DamC reveals principles of chromatin folding in vivo without crosslinking and ligation

Variable Extent of Lineage-Specificity and Developmental Stage-Specificity of Cohesin and CCCTC-Binding Factor Binding Within the Immunoglobulin and T Cell Receptor Loci

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

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