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ELF-MF exposure affects the robustness of epigenetic programming during granulopoiesis
JournalArticle (Originalarbeit in einer wissenschaftlichen Zeitschrift)
 
ID 3791475
Author(s) Manser, Melissa; Sater, Mohamad R. Abdul; Schmid, Christoph D.; Noreen, Faiza; Murbach, Manuel; Kuster, Niels; Schuermann, David; Schär, Primo
Author(s) at UniBasel Schär, Primo Leo
Year 2017
Title ELF-MF exposure affects the robustness of epigenetic programming during granulopoiesis
Journal Scientific Reports
Volume 7
Pages / Article-Number 43345
Abstract Extremely-low-frequency magnetic fields (ELF-MF) have been classified as "possibly carcinogenic" to humans on the grounds of an epidemiological association of ELF-MF exposure with an increased risk of childhood leukaemia. Yet, underlying mechanisms have remained obscure. Genome instability seems an unlikely reason as the energy transmitted by ELF-MF is too low to damage DNA and induce cancer-promoting mutations. ELF-MF, however, may perturb the epigenetic code of genomes, which is well-known to be sensitive to environmental conditions and generally deranged in cancers, including leukaemia. We examined the potential of ELF-MF to influence key epigenetic modifications in leukaemic Jurkat cells and in human CD34+ haematopoietic stem cells undergoing in vitro differentiation into the neutrophilic lineage. During granulopoiesis, sensitive genome-wide profiling of multiple replicate experiments did not reveal any statistically significant, ELF-MF-dependent alterations in the patterns of active (H3K4me2) and repressive (H3K27me3) histone marks nor in DNA methylation. However, ELF-MF exposure showed consistent effects on the reproducibility of these histone and DNA modification profiles (replicate variability), which appear to be of a stochastic nature but show preferences for the genomic context. The data indicate that ELF-MF exposure stabilizes active chromatin, particularly during the transition from a repressive to an active state during cell differentiation.
Publisher NATURE PUBLISHING GROUP
ISSN/ISBN 2045-2322
URL http://doi.org/10.1038/srep43345
edoc-URL https://edoc.unibas.ch/62081/
Full Text on edoc No
Digital Object Identifier DOI 10.1038/srep43345
PubMed ID http://www.ncbi.nlm.nih.gov/pubmed/28266526
ISI-Number WOS:000395624200001
Document type (ISI) Journal Article
 
   

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