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Literature DB >> 24861957

Chromatin maintenance and dynamics in senescence: a spotlight on SAHF formation and the epigenome of senescent cells.

Abstract

Senescence is a stable proliferation arrest characterized by profound changes in cellular morphology and metabolism as well as by extensive chromatin reorganization in the nucleus. One particular hallmark of chromatin changes during senescence is the formation of punctate DNA foci in DAPI-stained senescent cells that have been called senescence-associated heterochromatin foci (SAHF). While many advances have been made concerning our understanding of the effectors of senescence, how chromatin is reorganized and maintained in senescent cells has remained largely elusive. Because chromatin structure is inherently dynamic, senescent cells face the challenge of developing chromatin maintenance mechanisms in the absence of DNA replication in order to maintain the senescent phenotype. Here, we summarize and review recent findings shedding light on SAHF composition and formation via spatial repositioning of chromatin, with a specific focus on the role of lamin B1 for this process. In addition, we discuss the physiological implication of SAHF formation, the role of histone variants, and histone chaperones during senescence and also elaborate on the more general changes observed in the epigenome of the senescent cells.

Entities: Chemical Disease Gene

Mesh：

Substances：
Heterochromatin
Histones

Year: 2014 PMID： 24861957 DOI： 10.1007/s00412-014-0469-6

Source DB: PubMed Journal: Chromosoma ISSN： 0009-5915 Impact factor: 4.316

116 in total

1. The ATRX syndrome protein forms a chromatin-remodeling complex with Daxx and localizes in promyelocytic leukemia nuclear bodies.

Authors: Yutong Xue; Richard Gibbons; Zhijiang Yan; Dafeng Yang; Tarra L McDowell; Salvatore Sechi; Jun Qin; Sharleen Zhou; Doug Higgs; Weidong Wang
Journal: Proc Natl Acad Sci U S A Date: 2003-09-02 Impact factor: 11.205

2. Genome-scale profiling of histone H3.3 replacement patterns.

Authors: Yoshiko Mito; Jorja G Henikoff; Steven Henikoff
Journal: Nat Genet Date: 2005-09-11 Impact factor: 38.330

3. Epigenetic memory of an active gene state depends on histone H3.3 incorporation into chromatin in the absence of transcription.

Authors: Ray Kit Ng; J B Gurdon
Journal: Nat Cell Biol Date: 2007-12-09 Impact factor: 28.824

4. Analysis of protein turnover by quantitative SNAP-based pulse-chase imaging.

Authors: Dani L Bodor; Mariluz Gómez Rodríguez; Nuno Moreno; Lars E T Jansen
Journal: Curr Protoc Cell Biol Date: 2012-06

5. Oncogenic ras provokes premature cell senescence associated with accumulation of p53 and p16INK4a.

Authors: M Serrano; A W Lin; M E McCurrach; D Beach; S W Lowe
Journal: Cell Date: 1997-03-07 Impact factor: 41.582

6. A novel role for high-mobility group a proteins in cellular senescence and heterochromatin formation.

Authors: Masashi Narita; Masako Narita; Valery Krizhanovsky; Sabrina Nuñez; Agustin Chicas; Stephen A Hearn; Michael P Myers; Scott W Lowe
Journal: Cell Date: 2006-08-11 Impact factor: 41.582

7. Senescence-associated (beta)-galactosidase reflects an increase in lysosomal mass during replicative ageing of human endothelial cells.

Authors: D J Kurz; S Decary; Y Hong; J D Erusalimsky
Journal: J Cell Sci Date: 2000-10 Impact factor: 5.285

8. Definition of pRB- and p53-dependent and -independent steps in HIRA/ASF1a-mediated formation of senescence-associated heterochromatin foci.

Authors: Xiaofen Ye; Brad Zerlanko; Rugang Zhang; Neeta Somaiah; Marc Lipinski; Paolo Salomoni; Peter D Adams
Journal: Mol Cell Biol Date: 2007-01-22 Impact factor: 4.272

9. Lamin B1 fluctuations have differential effects on cellular proliferation and senescence.

Authors: Oliver Dreesen; Alexandre Chojnowski; Peh Fern Ong; Tian Yun Zhao; John E Common; Declan Lunny; E Birgitte Lane; Shu Jin Lee; Leah A Vardy; Colin L Stewart; Alan Colman
Journal: J Cell Biol Date: 2013-02-25 Impact factor: 10.539

10. Increased methylation variation in epigenetic domains across cancer types.

Authors: Kasper Daniel Hansen; Winston Timp; Héctor Corrada Bravo; Sarven Sabunciyan; Benjamin Langmead; Oliver G McDonald; Bo Wen; Hao Wu; Yun Liu; Dinh Diep; Eirikur Briem; Kun Zhang; Rafael A Irizarry; Andrew P Feinberg
Journal: Nat Genet Date: 2011-06-26 Impact factor: 38.330

18 in total

1. HSP90 inhibition alters the chemotherapy-driven rearrangement of the oncogenic secretome.

Authors: Simona di Martino; Carla Azzurra Amoreo; Barbara Nuvoli; Rossella Galati; Sabrina Strano; Francesco Facciolo; Gabriele Alessandrini; Harvey I Pass; Gennaro Ciliberto; Giovanni Blandino; Ruggero De Maria; Mario Cioce
Journal: Oncogene Date: 2018-01-09 Impact factor: 9.867

10. Nucleolus association of chromosomal domains is largely maintained in cellular senescence despite massive nuclear reorganisation.

Authors: Stefan Dillinger; Tobias Straub; Attila Németh
Journal: PLoS One Date: 2017-06-02 Impact factor: 3.240

Chromatin maintenance and dynamics in senescence: a spotlight on SAHF formation and the epigenome of senescent cells.

1. The ATRX syndrome protein forms a chromatin-remodeling complex with Daxx and localizes in promyelocytic leukemia nuclear bodies.

2. Genome-scale profiling of histone H3.3 replacement patterns.

3. Epigenetic memory of an active gene state depends on histone H3.3 incorporation into chromatin in the absence of transcription.

4. Analysis of protein turnover by quantitative SNAP-based pulse-chase imaging.

5. Oncogenic ras provokes premature cell senescence associated with accumulation of p53 and p16INK4a.

6. A novel role for high-mobility group a proteins in cellular senescence and heterochromatin formation.

7. Senescence-associated (beta)-galactosidase reflects an increase in lysosomal mass during replicative ageing of human endothelial cells.

8. Definition of pRB- and p53-dependent and -independent steps in HIRA/ASF1a-mediated formation of senescence-associated heterochromatin foci.

9. Lamin B1 fluctuations have differential effects on cellular proliferation and senescence.

10. Increased methylation variation in epigenetic domains across cancer types.

1. HSP90 inhibition alters the chemotherapy-driven rearrangement of the oncogenic secretome.

2. Retinoblastoma-binding Protein 4-regulated Classical Nuclear Transport Is Involved in Cellular Senescence.

3. HIF-1α and rapamycin act as gerosuppressant in multiple myeloma cells upon genotoxic stress.

4. Derepression of hTERT gene expression promotes escape from oncogene-induced cellular senescence.

Review 5. New Insights into the Regulation of Heterochromatin.

Review 6. Loss of chromatin structural integrity is a source of stress during aging.

7. Spatial reorganization of telomeres in long-lived quiescent cells.

Review 8. Linking replication stress with heterochromatin formation.

9. A Heterochromatin Domain Forms Gradually at a New Telomere and Is Dynamic at Stable Telomeres.

10. Nucleolus association of chromosomal domains is largely maintained in cellular senescence despite massive nuclear reorganisation.