TRIM28 repression of retrotransposon-based enhancers is necessary to preserve transcriptional dynamics in embryonic stem cells

Rowe, Helen M.; Kapopoulou, Adamandia; Corsinotti, Andrea; Fasching, Liana; Macfarlan, Todd S.; Tarabay, Yara; Viville, Stéphane; Jakobsson, Johan; Pfaff, Samuel L.; Trono, Didier

doi:10.1101/gr.147678.112

Cited by 147 publications

(177 citation statements)

References 75 publications

(107 reference statements)

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“…Despite their abundance, the functions of KRABZFPs have long remained ill-defined, although cumulated data have implicated some of them in processes as diverse as imprinting, cell differentiation, metabolic control and sexual dimorphism (reviewed by Lupo et al, 2013). This picture changed when the KRABbinding co-factor KAP1 was demonstrated to be essential for the early embryonic repression of TEs in both mouse and human, and when a few individual KRAB-ZFPs could be linked to this function as well Goff, 2007, 2009;Wolf et al, 2015b;Rowe et al, 2010Rowe et al, , 2013Jacobs et al, 2014). It was then suspected that the primary role of KRAB-ZFPs was to silence TEs, and that their evolutionary selection represented the host component of an arms race against these genetic invaders (Jacobs et al, 2014;Castro-Diaz et al, 2014;Thomas and Schneider, 2011).…”

Section: Introductionmentioning

confidence: 99%

KRAB zinc finger proteins

2017

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Krüppel-associated box domain zinc finger proteins (KRAB-ZFPs) are the largest family of transcriptional regulators in higher vertebrates. Characterized by an N-terminal KRAB domain and a C-terminal array of DNA-binding zinc fingers, they participate, together with their co-factor KAP1 (also known as TRIM28), in repression of sequences derived from transposable elements (TEs). Until recently, KRAB-ZFP/KAP1-mediated repression of TEs was thought to lead to irreversible silencing, and the evolutionary selection of KRAB-ZFPs was considered to be just the host component of an arms race against TEs. However, recent advances indicate that KRAB-ZFPs and their TE targets also partner up to establish speciesspecific regulatory networks. Here, we provide an overview of the KRAB-ZFP gene family, highlighting how its evolutionary history is linked to that of TEs, and how KRAB-ZFPs influence multiple aspects of development and physiology.

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Section: Introductionmentioning

confidence: 99%

KRAB zinc finger proteins

2017

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“…Chromatin was prepared from 10 7 H1 cells or primary CD4 + T-cells isolated from two donors as previously described (Rowe et al 2013b), and ChIP performed with rabbit anti-TRIM28 (SY 3267-68, 60 µL per IP, Tronolab) or Abcam anti-TRIM28 (for the hES-2 ChIPseq, ab10483, 5 µL per IP), anti-H3K9me3 (pAb-056-050, 1 µg/µL, 10 µL per IP, Diagenode), anti-SETDB1 (a kind gift from F. Rauscher, 5 µL per IP), and anti-H3K4me1 (pAb-037-050, 5 µL per IP, Diagenode) antibodies. All qPCRs were performed in triplicate with SYBR Green mix (Applied Biosystems) on IPed material and Total input (Ti) using primers listed in the Supplemental Material.…”

Section: Chromatin Immunoprecipitationmentioning

confidence: 99%

“…TRIM28 is also essential for the silencing of endogenous and some exogenous retroviruses in murine embryonic cells Goff 2007, 2009;Matsui et al 2010;Rowe et al 2010), where its KRAB-ZFP-mediated docking triggers the formation of heterochromatin, notably through the recruitment of SETDB1, the histone methyltransferase responsible for depositing the H3K9me3 repressive mark (Schultz et al 2002;Ivanov et al 2007;Frietze et al 2010), and of DNA methyltransferases, the action of which extends to adjacent CpG islands (Quenneville et al 2011(Quenneville et al , 2012Zuo et al 2012). A major consequence of the TRIM28-mediated repression of ERVs is the preservation of the transcription dynamics of murine ES cells, as repressive chromatin marks at murine ERVs are replaced upon Trim28 knockout by histone modifications typically found on active enhancers, which results in inducing the expression of nearby cellular genes, notably those harboring bivalent promoters (Rowe et al 2013b). …”

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Interplay of TRIM28 and DNA methylation in controlling human endogenous retroelements

et al. 2014

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Reverse transcription-derived sequences account for at least half of the human genome. Although these retroelements are formidable motors of evolution, they can occasionally cause disease, and accordingly are inactivated during early embryogenesis through epigenetic mechanisms. In the mouse, at least for endogenous retroviruses, important mediators of this process are the tetrapod-specific KRAB-containing zinc finger proteins (KRAB-ZFPs) and their cofactor TRIM28. The present study demonstrates that KRAB/TRIM28-mediated regulation is responsible for controlling a very broad range of human-specific endogenous retroelements (EREs) in human embryonic stem (ES) cells and that it exerts, as a consequence, a marked effect on the transcriptional dynamics of these cells. It further reveals reciprocal dependence between TRIM28 recruitment at specific families of EREs and DNA methylation. It finally points to the importance of persistent TRIM28-mediated control of ERE transcriptional impact beyond their presumed inactivation by DNA methylation.

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“…KAP1, also known as TRIM28 (tripartite motif protein 28), TIF1β (transcription intermediary factor 1 beta) or KRIP-1 (KRAB-interacting protein 1), acts as a scaffold for a multimolecular complex that silences transcription through the formation of heterochromatin (8)(9)(10)(11). The KRAB/KAP1 system probably evolved initially to minimize retroelement-induced genome perturbations (12)(13)(14), but recent data indicate that it also regulates multiple aspects of mammalian physiology (15)(16)(17)(18)(19)(20)(21)(22)(23)(24). The present study was undertaken to explore its role in hematopoiesis.…”

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A KRAB/KAP1-miRNA Cascade Regulates Erythropoiesis Through Stage-Specific Control of Mitophagy

Barde

Rauwel

Marin-Flórez

et al. 2013

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During hematopoiesis, lineage-and stage-specific transcription factors work in concert with chromatin modifiers to direct the differentiation of all blood cells. Here, we explored the role of KRAB-containing zinc finger proteins (KRAB-ZFPs) and their cofactor KAP1 in this process. Hematopoietic-restricted deletion of Kap1 in the mouse resulted in severe hypoproliferative anemia. Kap1-deleted erythroblasts failed to induce mitophagy-associated genes and retained mitochondria. This was due to persistent expression of microRNAs targeting mitophagy transcripts, itself secondary to a lack of repression by stage-specific KRAB-ZFPs. The KRAB/ KAP1-miRNA regulatory cascade is evolutionary conserved, as it also controls mitophagy during human erythropoiesis. Thus, a multilayered transcription regulatory system is present, where protein-and RNA-based repressors are super-imposed in combinatorial fashion to govern the timely triggering of an important differentiation event.Through the process of erythropoiesis, about one hundred billion new red cells are generated every day in the human adult bone marrow. This process is initiated by the differentiation of hematopoietic stem cells (HSC) into the earliest erythroid progenitor, which was identified ex vivo as a slowly growing burst-forming unit-erythroid (BFU-E). This erythroid progenitor morphs into the rapidly dividing CFU-E (colony-forming unit-erythroid), the proliferation of which is stimulated by the hypoxia-induced hormone erythropoietin. Further differentiation occurs through a highly sophisticated program orchestrated by lineage-and stage-specific combinations of protein-and RNA-based transcription regulators (1-3). It culminates in the elimination of intracellular organelles including mitochondria and the nucleus to yield the fully mature erythrocyte, containing on the order of 250 million molecules of hemoglobin as almost sole cargo. Much is still to be learned about the molecular mechanisms of these events, not only to understand the cause of red cell disorders, but also to aid the in vitro manufacturing of the large supplies of oxygen-carrying cells for transfusion.Higher vertebrate genomes encode hundreds of KRAB-ZFPs that can bind DNA in a sequence-specific fashion through a C-terminal array of C2H2 zinc fingers and recruit the ‡ Corresponding author. didier.trono@epfl.ch.

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TRIM28 repression of retrotransposon-based enhancers is necessary to preserve transcriptional dynamics in embryonic stem cells

Cited by 147 publications

References 75 publications

KRAB zinc finger proteins

KRAB zinc finger proteins

Interplay of TRIM28 and DNA methylation in controlling human endogenous retroelements

A KRAB/KAP1-miRNA Cascade Regulates Erythropoiesis Through Stage-Specific Control of Mitophagy

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