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Meiotic DNA double-strand break-independent role of protein phosphatase 4 in Hop1 assembly to promote meiotic chromosome axis formation in budding yeast
Authors:Ke Li  Kei Yoshimura  Miki Shinohara
Affiliation:1. Institute for Protein Research, Osaka University, Osaka, Japan

Department of Bioscience, Graduate School of Science, Osaka University, Osaka, Japan

Department of Advanced Bioscience, Graduate School of Agriculture, Kindai University, Nara, Japan;2. Department of Advanced Bioscience, Graduate School of Agriculture, Kindai University, Nara, Japan;3. Institute for Protein Research, Osaka University, Osaka, Japan

Abstract:Dynamic changes in chromosomal structure that occur during meiotic prophase play an important role in the progression of meiosis. Among them, meiosis-specific chromosomal axis-loop structures are important as a scaffold for integrated control between the meiotic recombination reaction and the associated checkpoint system to ensure accurate chromosome segregation. However, the molecular mechanism of the initial step of chromosome axis-loop construction is not well understood. Here, we showed that, in budding yeast, protein phosphatase 4 (PP4) that primarily counteracts Mec1/Tel1 phosphorylation is required to promote the assembly of a chromosomal axis component Hop1 and Red1 onto meiotic chromatin via interaction with Hop1. PP4, on the other hand, less affects Rec8 assembly. Notably, unlike the previously known function of PP4, this PP4 function in Hop1/Red1 assembly was independent of meiotic DSB-dependent Tel1/Mec1 kinase activities. The defect in Hop1/Red1 assembly in the absence of PP4 function was not suppressed by dysfunction of Pch2, which removes Hop1 protein from the chromosome axis, suggesting that PP4 is required for the initial step of chromatin loading of Hop1 rather than stabilization of Hop1 on axes. These results indicate phosphorylation/dephosphorylation-mediated regulation of Hop1 recruitment onto chromatin during chromosome axis construction before meiotic double-strand break formation.
Keywords:meiosis  meiotic chromosomal structure  meiotic recombination  Protein phosphatase 4
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