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Histone Variant H2A.Z Regulates Centromere Silencing and Chromosome Segregation in Fission Yeast
Authors:Haitong Hou   Yu Wang   Scott P. Kallgren   James Thompson   John R. Yates   III   Songtao Jia
Affiliation:From the Department of Biological Sciences, Columbia University, New York, New York 10027 and ;the §Department of Cell Biology, The Scripps Research Institute, La Jolla, California 92037
Abstract:The incorporation of histone variant H2A.Z into nucleosomes plays essential roles in regulating chromatin structure and gene expression. A multisubunit complex containing chromatin remodeling protein Swr1 is responsible for the deposition of H2A.Z in budding yeast and mammals. Here, we show that the JmjC domain protein Msc1 is a novel component of the fission yeast Swr1 complex and is required for Swr1-mediated incorporation of H2A.Z into nucleosomes at gene promoters. Loss of Msc1, Swr1, or H2A.Z results in loss of silencing at centromeres and defective chromosome segregation, although centromeric levels of CENP-A, a centromere-specific histone H3 variant that is required for setting up the chromatin structure at centromeres, remain unchanged. Intriguingly, H2A.Z is required for the expression of another centromere protein, CENP-C, and overexpression of CENP-C rescues centromere silencing defects associated with H2A.Z loss. These results demonstrate the importance of H2A.Z and CENP-C in maintaining a silenced chromatin state at centromeres.
Keywords:Chromatin/Epigenetics   Chromosomes/Centromeres   Genetics/Yeast   Histones   Centromeres   Chromatin Histone Modification   CENP-C   H2A.Z
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