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Literature DB >> 25107471

Dynamics of genomic H3K27me3 domains and role of EZH2 during pancreatic endocrine specification.

Cheng-Ran Xu¹, Lin-Chen Li², Greg Donahue³, Lei Ying⁴, Yu-Wei Zhang², Paul Gadue⁴, Kenneth S Zaret⁵.

Abstract

Endoderm cells undergo sequential fate choices to generate insulin-secreting beta cells. Ezh2 of the PRC2 complex, which generates H3K27me3, modulates the transition from endoderm to pancreas progenitors, but the role of Ezh2 and H3K27me3 in the next transition to endocrine progenitors is unknown. We isolated endoderm cells, pancreas progenitors, and endocrine progenitors from different staged mouse embryos and analyzed H3K27me3 genome-wide. Unlike the decline in H3K27me3 domains reported during embryonic stem cell differentiation in vitro, we find that H3K27me3 domains increase in number during endocrine progenitor development in vivo. Genes that lose the H3K27me3 mark typically encode transcriptional regulators, including those for pro-endocrine fates, whereas genes that acquire the mark typically are involved in cell biology and morphogenesis. Deletion of Ezh2 at the pancreas progenitor stage enhanced the production of endocrine progenitors and beta cells. Inhibition of EZH2 in embryonic pancreas explants and in human embryonic stem cell cultures increased endocrine progenitors in vitro. Our studies reveal distinct dynamics in H3K27me3 targets in vivo and a means to modulate beta cell development from stem cells.

Entities: Disease Gene Species

Keywords: Ezh2; H3K27me3; embryogenesis; endocrine; pancreas

Mesh：

Substances：

Year: 2014 PMID： 25107471 PMCID： PMC4282504 DOI： 10.15252/embj.201488671

Source DB: PubMed Journal: EMBO J ISSN： 0261-4189 Impact factor: 11.598

46 in total

1. Global expression analysis of gene regulatory pathways during endocrine pancreatic development.

Authors: Guoqiang Gu; James M Wells; David Dombkowski; Fred Preffer; Bruce Aronow; Douglas A Melton
Journal: Development Date: 2003-12-03 Impact factor: 6.868

2. Role of histone H3 lysine 27 methylation in Polycomb-group silencing.

Authors: Ru Cao; Liangjun Wang; Hengbin Wang; Li Xia; Hediye Erdjument-Bromage; Paul Tempst; Richard S Jones; Yi Zhang
Journal: Science Date: 2002-09-26 Impact factor: 47.728

3. High-resolution profiling of histone methylations in the human genome.

Authors: Artem Barski; Suresh Cuddapah; Kairong Cui; Tae-Young Roh; Dustin E Schones; Zhibin Wang; Gang Wei; Iouri Chepelev; Keji Zhao
Journal: Cell Date: 2007-05-18 Impact factor: 41.582

4. Transcription factor hepatocyte nuclear factor 6 regulates pancreatic endocrine cell differentiation and controls expression of the proendocrine gene ngn3.

Authors: P Jacquemin; S M Durviaux; J Jensen; C Godfraind; G Gradwohl; F Guillemot; O D Madsen; P Carmeliet; M Dewerchin; D Collen; G G Rousseau; F P Lemaigre
Journal: Mol Cell Biol Date: 2000-06 Impact factor: 4.272

5. The polycomb-group gene Ezh2 is required for early mouse development.

Authors: D O'Carroll; S Erhardt; M Pagani; S C Barton; M A Surani; T Jenuwein
Journal: Mol Cell Biol Date: 2001-07 Impact factor: 4.272

6. neurogenin3 is required for the development of the four endocrine cell lineages of the pancreas.

Authors: G Gradwohl; A Dierich; M LeMeur; F Guillemot
Journal: Proc Natl Acad Sci U S A Date: 2000-02-15 Impact factor: 11.205

7. Ezh2 controls B cell development through histone H3 methylation and Igh rearrangement.

Authors: I-Hsin Su; Ashwin Basavaraj; Andrew N Krutchinsky; Oliver Hobert; Axel Ullrich; Brian T Chait; Alexander Tarakhovsky
Journal: Nat Immunol Date: 2002-12-23 Impact factor: 25.606

8. Neurogenin 3 is essential for the proper specification of gastric enteroendocrine cells and the maintenance of gastric epithelial cell identity.

Authors: Catherine S Lee; Nathalie Perreault; John E Brestelli; Klaus H Kaestner
Journal: Genes Dev Date: 2002-06-15 Impact factor: 11.361

9. A bipotential precursor population for pancreas and liver within the embryonic endoderm.

Authors: G Deutsch; J Jung; M Zheng; J Lóra; K S Zaret
Journal: Development Date: 2001-03 Impact factor: 6.868

10. Direct evidence for the pancreatic lineage: NGN3+ cells are islet progenitors and are distinct from duct progenitors.

Authors: Guoqiang Gu; Jolanta Dubauskaite; Douglas A Melton
Journal: Development Date: 2002-05 Impact factor: 6.868

32 in total

Review 10. Monogenic Diabetes Modeling: In Vitro Pancreatic Differentiation From Human Pluripotent Stem Cells Gains Momentum.

Authors: Juan Ignacio Burgos; Ludovic Vallier; Santiago A Rodríguez-Seguí
Journal: Front Endocrinol (Lausanne) Date: 2021-07-06 Impact factor: 5.555

Dynamics of genomic H3K27me3 domains and role of EZH2 during pancreatic endocrine specification.

1. Global expression analysis of gene regulatory pathways during endocrine pancreatic development.

2. Role of histone H3 lysine 27 methylation in Polycomb-group silencing.

3. High-resolution profiling of histone methylations in the human genome.

4. Transcription factor hepatocyte nuclear factor 6 regulates pancreatic endocrine cell differentiation and controls expression of the proendocrine gene ngn3.

5. The polycomb-group gene Ezh2 is required for early mouse development.

6. neurogenin3 is required for the development of the four endocrine cell lineages of the pancreas.

7. Ezh2 controls B cell development through histone H3 methylation and Igh rearrangement.

8. Neurogenin 3 is essential for the proper specification of gastric enteroendocrine cells and the maintenance of gastric epithelial cell identity.

9. A bipotential precursor population for pancreas and liver within the embryonic endoderm.

10. Direct evidence for the pancreatic lineage: NGN3+ cells are islet progenitors and are distinct from duct progenitors.

1. Differentially Expressed MicroRNA-483 Confers Distinct Functions in Pancreatic β- and α-Cells.

2. Single-cell transcriptomic analyses reveal distinct dorsal/ventral pancreatic programs.

3. Taming the young and restless--epigenetic gene regulation in pancreas and beta-cell precursors.

4. H3K27me3 is an Epigenetic Mark of Relevance in Endometriosis.

5. Genomic and Proteomic Resolution of Heterochromatin and Its Restriction of Alternate Fate Genes.

Review 6. Epigenetic modifications and long noncoding RNAs influence pancreas development and function.

7. Dnmt1 activity is dispensable in δ-cells but is essential for α-cell homeostasis.

Review 8. A systems view of epigenetic networks regulating pancreas development and β-cell function.

Review 9. H3K9me3-Dependent Heterochromatin: Barrier to Cell Fate Changes.

Review 10. Monogenic Diabetes Modeling: In Vitro Pancreatic Differentiation From Human Pluripotent Stem Cells Gains Momentum.