Literature DB >> 18297071

Crossover assurance and crossover interference are distinctly regulated by the ZMM proteins during yeast meiosis.

Miki Shinohara1, Steve D Oh, Neil Hunter, Akira Shinohara.   

Abstract

Meiotic crossing-over is highly regulated such that each homolog pair typically receives at least one crossover (assurance) and adjacent crossovers are widely spaced (interference). Here we provide evidence that interference and assurance are mechanistically distinct processes that are separated by mutations in a new ZMM (Zip, Msh, Mer) protein from Saccharomyces cerevisiae, Spo16. Like other zmm mutants, spo16 cells have defects in both crossing-over and synaptonemal complex formation. Unlike in previously characterized zmm mutants, the residual crossovers in spo16 cells show interference comparable to that in the wild type. Spo16 interacts with a second ZMM protein, Spo22 (also known as Zip4), and spo22 mutants also show normal interference. Notably, assembly of the MutS homologs Msh4 and Msh5 on chromosomes occurs in both spo16 and spo22, but not in other zmm mutants. We suggest that crossover interference requires the normal assembly of recombination complexes containing Msh4 and Msh5 but does not require Spo16- and Spo22-dependent extension of synaptonemal complexes. In contrast, crossover assurance requires all ZMM proteins and full-length synaptonemal complexes.

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Year:  2008        PMID: 18297071     DOI: 10.1038/ng.83

Source DB:  PubMed          Journal:  Nat Genet        ISSN: 1061-4036            Impact factor:   38.330


  106 in total

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6.  Common and low-frequency variants associated with genome-wide recombination rate.

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8.  Replication protein A2c coupled with replication protein A1c regulates crossover formation during meiosis in rice.

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9.  The conserved XPF:ERCC1-like Zip2:Spo16 complex controls meiotic crossover formation through structure-specific DNA binding.

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10.  The synaptonemal complex protein, Zip1, promotes the segregation of nonexchange chromosomes at meiosis I.

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