Co-optation of Tandem DNA Repeats for the Maintenance of Mesenchymal Identity

Balestrieri, Chiara; Alfarano, Gabriele; Milan, Marta; Tosi, Valentina; Prosperini, Elena; Nicoli, Paola; Palamidessi, Andrea; Scita, Giorgio; Diaferia, Giuseppe R.; Natoli, Gioacchino

doi:10.1016/j.cell.2018.03.081

Cited by 32 publications

(32 citation statements)

References 78 publications

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“…In the context of an effort to determine how the transcriptional networks operating in exocrine pancreas are rewired in PDACs (Diaferia et al, 2016;Balestrieri et al, 2018), we report here that while FOXA1 and FOXA2 are co-expressed in well-differentiated PDAC cells, they are dissociated in the less differentiated cellular component, in which only FOXA2 is expressed, albeit nonuniformly. This dissociation is reminiscent of normal embryonic development, in which FOXA2 is expressed before FOXA1 (Sasaki & Hogan, 1993), thus explaining the inability of the latter to ◀ Figure 6.…”

Section: Discussionmentioning

confidence: 94%

“…ChIP-seq was carried out using previously described protocols (Curina et al, 2017;Balestrieri et al, 2018) on an Illumina HiSeq 2000 platform. 10 6 (H3K27ac) or 50-150 × 10 6 (TFs) were either fixed with formaldehyde as described before (for H3K27ac, FOXA2, HOXB8, and JUNB ChIP-seq) or fixed with a double cross-linking protocol (for FOS ChIP-seq).…”

Section: Chip-seqmentioning

confidence: 99%

“…DNA was either purified with QIAquick columns (Qiagen) or solid-phase reversible immobilization (SPRI) beads (Agencourt AMPure XP, Beckman Coulter) and then quantified with QuantiFluor (Promega). DNA libraries were prepared for HiSeq 2000 or NextSeq 500 sequencing as described (Balestrieri et al, 2018).…”

Section: Chip-seqmentioning

confidence: 99%

“…We have recently undertaken a systematic effort aiming at dissecting the transcriptional regulatory networks underlying alterations of differentiation in human PDAC (Diaferia et al, 2016;Balestrieri et al, 2018). Together with TFs expressed irrespective of cytological differentiation, we identified and initially characterized a panel of TFs selectively expressed or active in either low-grade (epithelial and well-differentiated) or high-grade (quasi-mesenchymal and poorly differentiated) PDAC cells (Diaferia et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

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FOXA 2 controls the cis ‐regulatory networks of pancreatic cancer cells in a differentiation grade‐specific manner

et al. 2019

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Differentiation of normal and tumor cells is controlled by regulatory networks enforced by lineage‐determining transcription factors (TFs). Among them, TFs such as FOXA1/2 bind naïve chromatin and induce its accessibility, thus establishing new gene regulatory networks. Pancreatic ductal adenocarcinoma (PDAC) is characterized by the coexistence of well‐ and poorly differentiated cells at all stages of disease. How the transcriptional networks determining such massive cellular heterogeneity are established remains to be determined. We found that FOXA2, a TF controlling pancreas specification, broadly contributed to the cis‐regulatory networks of PDACs. Despite being expressed in both well‐ and poorly differentiated PDAC cells, FOXA2 displayed extensively different genomic distributions and controlled distinct gene expression programs. Grade‐specific functions of FOXA2 depended on its partnership with TFs whose expression varied depending on the differentiation grade. These data suggest that FOXA2 contributes to the regulatory networks of heterogeneous PDAC cells via interactions with alternative partner TFs.

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Section: Discussionmentioning

confidence: 94%

Section: Chip-seqmentioning

confidence: 99%

Section: Chip-seqmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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FOXA 2 controls the cis ‐regulatory networks of pancreatic cancer cells in a differentiation grade‐specific manner

et al. 2019

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“…In this study, we found that two enhancers in the mouse genome exhibit an exceptional density of PU.1 motifs, which are triggers for outlier levels of TRIM33 recruitment to cause repression of neighboring genes Bim and Atp1b3 (Wang et al, 2015a). In a recent study, it was found that DNA replication errors can produce tandem repeats to produce homotypic TF binding sites, which can promote the evolution of novel cis -regulatory elements (Balestrieri et al, 2018). Based on these findings, we propose that homotypic motif clustering as a general mechanism by which transcription factors and cofactors become endowed with high-precision regulatory functions during evolution.…”

Section: Discussionmentioning

confidence: 99%

A Transcription Factor Addiction in Leukemia Imposed by the MLL Promoter Sequence

et al. 2018

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Summary The Mixed Lineage Leukemia gene (MLL) is altered in leukemia by chromosomal translocations to produce oncoproteins comprised of the MLL N-terminus fused to the C-terminus of a partner protein. Here, we used domain-focused CRISPR screening to identify ZFP64 as an essential transcription factor in MLL-rearranged leukemia. We show that the critical function of ZFP64 in leukemia is to maintain MLL expression via binding to the MLL promoter, which is the most enriched location of ZFP64 occupancy in the human genome. The specificity of ZFP64 for MLL is accounted for by an exceptional density of ZFP64 motifs embedded within the MLL promoter. These findings demonstrate how a sequence anomaly of an oncogene promoter can impose a transcriptional addiction in cancer.

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Absence of CG methylation alters the long noncoding transcriptome landscape in multiple species

et al. 2021

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The noncoding regions throughout the genome are in large part comprised of transposable elements (TEs), some of which are functionalized with long intergenic noncoding RNAs (lincRNAs). DNA methylation is predominantly associated with TEs, but little is known about its contribution to the transcription of lincRNAs. Here, we examine the lincRNA profiles of DNA methylation-related mutants of five species, Arabidopsis, rice, tomato, maize, and mouse, to elucidate patterns in lincRNA regulation under altered DNA methylation status. Significant activation of lincRNAs was observed in the absence of CG DNA methylation rather than non-CG. Our study establishes a working model of the contribution of DNA methylation to regulation of the dynamic activity of lincRNA transcription.

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Co-optation of Tandem DNA Repeats for the Maintenance of Mesenchymal Identity

Cited by 32 publications

References 78 publications

FOXA 2 controls the cis ‐regulatory networks of pancreatic cancer cells in a differentiation grade‐specific manner

FOXA 2 controls the cis ‐regulatory networks of pancreatic cancer cells in a differentiation grade‐specific manner

A Transcription Factor Addiction in Leukemia Imposed by the MLL Promoter Sequence

Absence of CG methylation alters the long noncoding transcriptome landscape in multiple species

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