Epigenetic mechanisms enable cells to develop novel adaptive phenotypes without altering their genetic blueprint. Recent studies show histone modifications, such as heterochromatin-defining H3K9 methylation (H3K9me), can be redistributed to establish adaptive phenotypes. We developed a precision-engineered genetic approach to trigger heterochromatin misregulation on-demand in fission yeast. This enabled us to trace genome-scale RNA and H3K9me changes over time in long-term, continuous cultures. Adaptive H3K9me establishes over remarkably slow timescales relative to the initiating stress. We captured dynamic H3K9me redistribution events which depend on an RNA binding complex MTREC, ultimately leading to cells converging on an optimal adaptive solution. Upon stress removal, cells relax to new transcriptional and chromatin states, establishing memory that is tunable and primed for future adaptive epigenetic responses. Collectively, we identify the slow kinetics of epigenetic adaptation that allow cells to discover and heritably encode novel adaptive solutions, with implications for drug resistance and response to infection.
Mapping the dynamics of epigenetic adaptation in S. pombe during heterochromatin misregulation.
绘制裂殖酵母异染色质失调过程中表观遗传适应的动态图谱
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作者:Larkin Ajay, Kunze Colin, Seman Melissa, Levashkevich Alexander, Curran Justin, Morris-Evans Dionysus, Lemieux Sophia, Khalil Ahmad S, Ragunathan Kaushik
| 期刊: | Developmental Cell | 影响因子: | 8.700 |
| 时间: | 2024 | 起止号: | 2024 Aug 19; 59(16):2222-2238 |
| doi: | 10.1016/j.devcel.2024.07.006 | 研究方向: | 表观遗传 |
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