| Literature DB >> 30457103 |
Kenneth Kh Ng1,2, Mary A Yui2, Arnav Mehta2, Sharmayne Siu3, Blythe Irwin1, Shirley Pease2, Satoshi Hirose2, Michael B Elowitz2,4, Ellen V Rothenberg2, Hao Yuan Kueh1,2.
Abstract
Cell fate decisions occur through the switch-like, irreversible activation of fate-specifying genes. These activation events are often assumed to be tightly coupled to changes in upstream transcription factors, but could also be constrained by cis-epigenetic mechanisms at individual gene loci. Here, we studied the activation of Bcl11b, which controls T-cell fate commitment. To disentangle cis and trans effects, we generated mice where two Bcl11b copies are tagged with distinguishable fluorescent proteins. Quantitative live microscopy of progenitors from these mice revealed that Bcl11b turned on after a stochastic delay averaging multiple days, which varied not only between cells but also between Bcl11b alleles within the same cell. Genetic perturbations, together with mathematical modeling, showed that a distal enhancer controls the rate of epigenetic activation, while a parallel Notch-dependent trans-acting step stimulates expression from activated loci. These results show that developmental fate transitions can be controlled by stochastic cis-acting events on individual loci.Entities:
Keywords: computational biology; developmental biology; epigenetics; gene regulation; lymphocyte development; mouse; quantitative and systems biology; stochastic gene expression; systems biology
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Year: 2018 PMID: 30457103 PMCID: PMC6245732 DOI: 10.7554/eLife.37851
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140