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Condensin I protects meiotic cohesin from WAPL-1 mediated removal.

Margarita R HernandezMichael B DavisJianhao JiangElizabeth A BrouhardAaron F SeversonGyörgyi Csankovszki
Published in: PLoS genetics (2018)
Condensin complexes are key determinants of higher-order chromatin structure and are required for mitotic and meiotic chromosome compaction and segregation. We identified a new role for condensin in the maintenance of sister chromatid cohesion during C. elegans meiosis. Using conventional and stimulated emission depletion (STED) microscopy we show that levels of chromosomally-bound cohesin were significantly reduced in dpy-28 mutants, which lack a subunit of condensin I. SYP-1, a component of the synaptonemal complex central region, was also diminished, but no decrease in the axial element protein HTP-3 was observed. Surprisingly, the two key meiotic cohesin complexes of C. elegans were both depleted from meiotic chromosomes following the loss of condensin I, and disrupting condensin I in cohesin mutants increased the frequency of detached sister chromatids. During mitosis and meiosis in many organisms, establishment of cohesion is antagonized by cohesin removal by Wapl, and we found that condensin I binds to C. elegans WAPL-1 and counteracts WAPL-1-dependent cohesin removal. Our data suggest that condensin I opposes WAPL-1 to promote stable binding of cohesin to meiotic chromosomes, thereby ensuring linkages between sister chromatids in early meiosis.
Keyphrases
  • gene expression
  • dna damage
  • single molecule
  • transcription factor
  • electronic health record
  • cell cycle
  • dna methylation
  • high throughput
  • optical coherence tomography
  • binding protein
  • mass spectrometry
  • copy number