BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs3825942, LEP, T cell receptor signaling pathway, Breast Cancer, Hippocampus)
Bookmark Forward

Meiotic prophase length modulates Tel1-dependent DNA double-strand break interference.

Luz María López Ruiz, Dominic Johnson, William H Gittens, George G B Brown, Rachal M Allison, Matthew J Neale

PLoS genetics 2024 Mar


filter terms:
  • dna breaks (1)
  • dna damage (1)
  • endodeoxyribonucleases (2)
  • kinases (2)
  • meiosis (2)
  • NDT80 (3)
  • peptides (2)
  • Spo11 (6)
  • strand breaks (14)
  • Tel1 (5)
    • Sizes of these terms reflect their relevance to your search.

    During meiosis, genetic recombination is initiated by the formation of many DNA double-strand breaks (DSBs) catalysed by the evolutionarily conserved topoisomerase-like enzyme, Spo11, in preferred genomic sites known as hotspots. DSB formation activates the Tel1/ATM DNA damage responsive (DDR) kinase, locally inhibiting Spo11 activity in adjacent hotspots via a process known as DSB interference. Intriguingly, in S. cerevisiae, over short genomic distances (<15 kb), Spo11 activity displays characteristics of concerted activity or clustering, wherein the frequency of DSB formation in adjacent hotspots is greater than expected by chance. We have proposed that clustering is caused by a limited number of sub-chromosomal domains becoming primed for DSB formation. Here, we provide evidence that DSB clustering is abolished when meiotic prophase timing is extended via deletion of the NDT80 transcription factor. We propose that extension of meiotic prophase enables most cells, and therefore most chromosomal domains within them, to reach an equilibrium state of similar Spo11-DSB potential, reducing the impact that priming has on estimates of coincident DSB formation. Consistent with this view, when Tel1 is absent but Ndt80 is present and thus cells are able to rapidly exit meiotic prophase, genome-wide maps of Spo11-DSB formation are skewed towards pericentromeric regions and regions that load pro-DSB factors early-revealing regions of preferential priming-but this effect is abolished when NDT80 is deleted. Our work highlights how the stochastic nature of Spo11-DSB formation in individual cells within the limited temporal window of meiotic prophase can cause localised DSB clustering-a phenomenon that is exacerbated in tel1Δ cells due to the dual roles that Tel1 has in DSB interference and meiotic prophase checkpoint control. Copyright: © 2024 López Ruiz et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

    Citation

    Luz María López Ruiz, Dominic Johnson, William H Gittens, George G B Brown, Rachal M Allison, Matthew J Neale. Meiotic prophase length modulates Tel1-dependent DNA double-strand break interference. PLoS genetics. 2024 Mar;20(3):e1011140

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 38427688

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.