Journal
GENETICS
Volume 181, Issue 1, Pages 39-51Publisher
GENETICS SOCIETY AMERICA
DOI: 10.1534/genetics.108.093112
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Funding
- Busch Foundation
- National Science Foundation
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During meiosis, programmed DNA double-strand breaks (DSBs) are repaired to create at least one crossover per chromosome arm. Crossovers mature into chiasmata, which hold and Orient the homologous chromosomes on file meiotic spindle to ensure proper segregation at meiosis I. This process is Usually monitored by one or more checkpoints that ensure that DSBs are repaired prior to the meiotic divisions. We show here that mutations in Drosophila genes required to process DSBs into crossovers delay two important steps in meiotic progression: a chromatin-remodeling process associated with DSB formation and the final steps of oocyte selection. Consistent with the hypothesis that a checkpoint has been activated, the delays in meiotic progression are suppressed 1)), a mutation in the Drosophila homolog of pch2. The PCH2-dependent delays also require proteins thought to regulate the number and distribution Of Crossovers, suggesting that this checkpoint Monitors events leading to crossover formation. Surprisingly, two lines of evidence suggest that the PCH2-dependent checkpoint does not reflect the accumulation of unprocessed recombination intermediates: the delays in meiotic progression do not depend oil DSB formation or on mei-41, the Drosophila ATR homolog, which is required for the checkpoint response to unrepaired DSBs. We propose that the sites and/or conditions required to promote crossovers are established independently of DSB formation early in meiotic prophase. Furthermore, the PCH2-dependent checkpoint is activated by these events and pachytene progression is delayed Until the DSB repair complexes required to generate crossovers are assembled. Interestingly, PCH2-dependent. delays in prophase may allow additional crossovers to form.
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