3D chromatin remodeling potentiates transcriptional programs driving cell invasion

Lebeau, Benjamin; Jangal, Maïka; Zhao, Tiejun; Wong, C. K.; Wong, Nolan; Cañedo, Eduardo Cepeda; Hebert, Steven C.; Aguilar‐Mahecha, Adriana; Chabot, Catherine; Buchanan, Marguerite; Catterall, Rachel; McCaffrey, Luke; Deblois, Geneviève; Kleinman, Claudia L.; Park, Morag; Basik, Mark; Witcher, Michael

doi:10.1073/pnas.2203452119

Cited by 9 publications

(10 citation statements)

References 103 publications

(165 reference statements)

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“…To understand the interplay between CTCF expression and binding, we analyzed the publicly available CTCF ChIP-seq data of CTCF knockdown in MCF10A from Lebeau et al. ( 55 ), in which they showed a 50–60% reduction in CTCF protein, and the overall CTCF binding of the cells remained largely unchanged, with a small number of lost CTCF binding sites, and even smaller number of gained CTCF binding sites ( 55 ). Reanalyzing their CTCF ChIP-seq data (alignment to the human GRCh38/hg38 build genome) and filtering out non-CTCF motif-containing binding sites, we found very similar results with a total of 38 875 CTCF peaks, of which 3270 were significantly lost (FDR < 0.01, log 2 FC < −1) and 504 CTCF peaks significantly gained (FDR < 0.01, log 2 FC > 1) in the CTCF knockdown cells, while the rest of CTCF binding peaks ( n = 35 101) remained statistically unchanged ( 55 ) (Figure 4A ).…”

Section: Resultsmentioning

confidence: 99%

“…The publicly available data for CTCF chromatin immunoprecipitation sequencing (ChIP-seq) from HeLa ( 45 ), GM12878 ( 45 ), MCF10A ( 54 , 55 ), Jurkat ( 56 ), NPCs ( 45 ) and RPE-1 ( 45 ), and each associated input control data, were downloaded and aligned to the GRCh38/hg38 genome using bowtie2 (v. 2.3.4.1). Binding peaks were called by the macs2 tool (v. 2.2.9.1) using the default setting with each dataset controlled for the matching input data (-c).…”

Section: Methodsmentioning

confidence: 99%

“…CTCF ChIP-seq data from MCF10A CTCF wild-type (WT) and knockdown (KD) cells ( 55 ) were downloaded and processed as described earlier. Binding peaks with CTCF motifs were used for further analysis to identify differentially binding regions using DiffBind 3.0 with the same parameters as described in Lebeau et al.…”

Section: Methodsmentioning

confidence: 99%

“…Binding peaks with CTCF motifs were used for further analysis to identify differentially binding regions using DiffBind 3.0 with the same parameters as described in Lebeau et al. ( 55 ). Briefly, bam and narrowPeak files for each sample and bam files of the associated input were used.…”

Section: Methodsmentioning

confidence: 99%

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DNA fragility at topologically associated domain boundaries is promoted by alternative DNA secondary structure and topoisomerase II activity

Raimer Young,

Hou,

Bartosik

et al. 2024

Nucleic Acids Research

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CCCTC-binding factor (CTCF) binding sites are hotspots of genome instability. Although many factors have been associated with CTCF binding site fragility, no study has integrated all fragility-related factors to understand the mechanism(s) of how they work together. Using an unbiased, genome-wide approach, we found that DNA double-strand breaks (DSBs) are enriched at strong, but not weak, CTCF binding sites in five human cell types. Energetically favorable alternative DNA secondary structures underlie strong CTCF binding sites. These structures coincided with the location of topoisomerase II (TOP2) cleavage complex, suggesting that DNA secondary structure acts as a recognition sequence for TOP2 binding and cleavage at CTCF binding sites. Furthermore, CTCF knockdown significantly increased DSBs at strong CTCF binding sites and at CTCF sites that are located at topologically associated domain (TAD) boundaries. TAD boundary-associated CTCF sites that lost CTCF upon knockdown displayed increased DSBs when compared to the gained sites, and those lost sites are overrepresented with G-quadruplexes, suggesting that the structures act as boundary insulators in the absence of CTCF, and contribute to increased DSBs. These results model how alternative DNA secondary structures facilitate recruitment of TOP2 to CTCF binding sites, providing mechanistic insight into DNA fragility at CTCF binding sites.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

DNA fragility at topologically associated domain boundaries is promoted by alternative DNA secondary structure and topoisomerase II activity

Raimer Young,

Hou,

Bartosik

et al. 2024

Nucleic Acids Research

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“…CTCF involvement in cell migration is ambiguous; on one hand it was shown to repress breast cancer cell migration and invasion 35,36 , while on the other hand it was shown to support migration and/or invasion of various primary and cancerous cells including human corneal epithelial cells 37,38 , cortical neurons 39 , skin-resident dendritic cells 40 , prostate cancer cells 41,42 , ovarian cancer cells 43 , gastric cancer cells 44 and melanoma cells 45 . Although it is assumed that CTCF affects cell migration by its ability to regulate transcription, the exact mechanism by which CTCF controls transcription to control cell migration has not been determined yet.…”

Section: Introductionmentioning

confidence: 99%

The CTCF-H3K27me3 axis supports melanoma cell migration by repressing cholesterol biosynthesis

Kaczmarczyk

Levi

Salmon‐Divon

et al. 2023

Preprint

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CCCTC-binding factor (CTCF) is a zinc finger protein that regulates correct three-dimensional chromatin folding in addition to activation and repression of transcription and splicing. CTCF was found to affect tumor cell migration, however the molecular mechanism is still obscure. To identify the molecular mechanism by which CTCF supports melanoma cell migration we used mouse melanoma cells with a partial loss of function (pLoF) of CTCF generated by the CRISPR-Cas9 system. Here we show that CTCF pLoF inhibited cell migration rate. Using RNA sequencing we identified an increase in the expression of multiple enzymes in the cholesterol biosynthesis pathway along with an increase in the cellular cholesterol levels. Inhibition of cholesterol synthesis in CTCF pLoF cells by Fatostatin restored the cellular migration rate, suggesting that CTCF supports cell migration by inhibition of cholesterol synthesis. Detailed analysis of the promoter of Hmgcs1, an upstream enzyme in the cholesterol synthesis pathway, revealed that CTCF pLoF led to reduced H3K27me3 levels in parallel to increased binding of the transcriptional activator SREBP2. Moreover, inhibition of H3K27 methylation in wildtype cells led to increased SREBP2 binding to this promoter. Taken together, our results suggest that CTCF represses transcription of Hmgc1 by promoting H3K27 methylation to suppress SREBP2 binding. By that, CTCF fine tune the cellular cholesterol levels to support cell migration.

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Hypoxia-induced CTCF promotes EMT in breast cancer

Kakani,

Dhamdhere,

Pant

et al. 2024

Cell Reports

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3D chromatin remodeling potentiates transcriptional programs driving cell invasion

Cited by 9 publications

References 103 publications

DNA fragility at topologically associated domain boundaries is promoted by alternative DNA secondary structure and topoisomerase II activity

DNA fragility at topologically associated domain boundaries is promoted by alternative DNA secondary structure and topoisomerase II activity

The CTCF-H3K27me3 axis supports melanoma cell migration by repressing cholesterol biosynthesis

Hypoxia-induced CTCF promotes EMT in breast cancer

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