EED, a member of the polycomb group, is required for nephron differentiation and the maintenance of nephron progenitor cells

Zhang, Le; Ettou, Sandrine; Khalid, Myda; Taglienti, Mary; Jain, Dhawal; Jung, Youngsook L.; Seager, Catherine M.; Liu, Yongqing; Ng, Kar Hui; Park, Peter J.; Kreidberg, Jordan A.

doi:10.1242/dev.157149

Cited by 15 publications

(16 citation statements)

References 47 publications

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“…The results of this work as well as previous works suggest that epigenetic mechanisms play a role in kidney development [ 30 , 40 , 41 , 42 , 43 , 44 , 45 ]. Therefore, we wanted to systematically evaluate the effect of epigenetic modulators of the different enzyme classes on renal development.…”

Section: Resultssupporting

confidence: 84%

Effects of Environmental Conditions on Nephron Number: Modeling Maternal Disease and Epigenetic Regulation in Renal Development

Fuhrmann

Lindner

Hauser

et al. 2021

IJMS

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A growing body of evidence suggests that low nephron numbers at birth can increase the risk of chronic kidney disease or hypertension later in life. Environmental stressors, such as maternal malnutrition, medication and smoking, can influence renal size at birth. Using metanephric organ cultures to model single-variable environmental conditions, models of maternal disease were evaluated for patterns of developmental impairment. While hyperthermia had limited effects on renal development, fetal iron deficiency was associated with severe impairment of renal growth and nephrogenesis with an all-proximal phenotype. Culturing kidney explants under high glucose conditions led to cellular and transcriptomic changes resembling human diabetic nephropathy. Short-term high glucose culture conditions were sufficient for long-term alterations in DNA methylation-associated epigenetic memory. Finally, the role of epigenetic modifiers in renal development was tested using a small compound library. Among the selected epigenetic inhibitors, various compounds elicited an effect on renal growth, such as HDAC (entinostat, TH39), histone demethylase (deferasirox, deferoxamine) and histone methyltransferase (cyproheptadine) inhibitors. Thus, metanephric organ cultures provide a valuable system for studying metabolic conditions and a tool for screening for epigenetic modifiers in renal development.

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Section: Resultssupporting

confidence: 84%

Effects of Environmental Conditions on Nephron Number: Modeling Maternal Disease and Epigenetic Regulation in Renal Development

Fuhrmann

Lindner

Hauser

et al. 2021

IJMS

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“…We speculate that these maturational changes in chromatin accessibility are likely orchestrated by concomitant changes in the epigenetic machinery such as the Polycomb complex, ATP-dependent chromatin remodelers, DNA methylation and the NuRD/HDAC complex, that govern the access of master regulators to their cis-acting elements. Indeed, there is genetic evidence that perturbations of the epigenetic machinery disrupt the balance between NPC proliferation and differentiation in vivo (Denner and Rauchman, 2013; El-Dahr and Saifudeen, 2018; Liu et al, 2018; Zhang et al, 2018). A caveat in this study is that ChIP-seq was performed on E13 and P0 NPC cultured in NPEM for two passages.…”

Section: Discussionmentioning

confidence: 99%

Defining the dynamic chromatin landscape of mouse nephron progenitors

et al. 2019

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Six2 + cap mesenchyme cells, also called nephron progenitor cells (NPC), are precursors of all epithelial cell types of the nephron, the filtering unit of the kidney. Current evidence indicates that perinatal ‘old’ NPC have a greater tendency to exit the progenitor niche and differentiate into nascent nephrons than their embryonic ‘young’ counterpart. Understanding the underpinnings of NPC development may offer insights to rejuvenate old NPC and expand the progenitor pool. Here, we compared the chromatin landscape of young and old NPC and found common features reflecting their shared lineage but also intrinsic differences in chromatin accessibility and enhancer landscape supporting the view that old NPC are epigenetically poised for differentiation. Annotation of open chromatin regions and active enhancers uncovered the transcription factor Bach2 as a potential link between the pro-renewal MAPK/AP1 and pro-differentiation Six2/b-catenin pathways that might be of critical importance in regulation of NPC fate. Our data provide the first glimpse of the dynamic chromatin landscape of NPC and serve as a platform for future studies of the impact of genetic or environmental perturbations on the epigenome of NPC.

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“…Eed KO resulted in smaller kidneys and premature loss of NPCs, and the investigators revealed a dual role of PRC2: it is required to maintain self-renewal of the NPCs; during differentiation, it might also be involved in repressing self-renewal genes, like Six2, to facilitate proper nephron differentiation. 15 However, the direct target genes regulated by PRC2 remains to be determined.…”

Section: Significance Statementmentioning

confidence: 99%

Epigenetic regulation of kidney progenitor cells

Huang

Liu

Vonk

et al. 2020

Stem Cells Translational Medicine

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The reciprocal interactions among the different embryonic kidney progenitor populations lay the basis for proper kidney organogenesis. During kidney development, three types of progenitor cells, including nephron progenitor cells, ureteric bud progenitor cells, and interstitial progenitor cells, generate the three major kidney structures-the nephrons, the collecting duct network, and the stroma, respectively. Epigenetic mechanisms are well recognized for playing important roles in organism development, in fine-tuned control of physiological activities, and in responses to environment stimuli. Recently, evidence supporting the importance of epigenetic mechanisms underlying kidney organogenesis has emerged. In this perspective, we summarize the research progress and discuss the potential contribution of novel stem cell, organoid, and next-generation sequencing tools in advancing this field in the future.

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EED, a member of the polycomb group, is required for nephron differentiation and the maintenance of nephron progenitor cells

Cited by 15 publications

References 47 publications

Effects of Environmental Conditions on Nephron Number: Modeling Maternal Disease and Epigenetic Regulation in Renal Development

Effects of Environmental Conditions on Nephron Number: Modeling Maternal Disease and Epigenetic Regulation in Renal Development

Defining the dynamic chromatin landscape of mouse nephron progenitors

Epigenetic regulation of kidney progenitor cells

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