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Molecular basis of CENP-C association with the CENP-A nucleosome at yeast centromeres.


ABSTRACT: Histone CENP-A-containing nucleosomes play an important role in nucleating kinetochores at centromeres for chromosome segregation. However, the molecular mechanisms by which CENP-A nucleosomes engage with kinetochore proteins are not well understood. Here, we report the finding of a new function for the budding yeast Cse4/CENP-A histone-fold domain interacting with inner kinetochore protein Mif2/CENP-C. Strikingly, we also discovered that AT-rich centromere DNA has an important role for Mif2 recruitment. Mif2 contacts one side of the nucleosome dyad, engaging with both Cse4 residues and AT-rich nucleosomal DNA. Both interactions are directed by a contiguous DNA- and histone-binding domain (DHBD) harboring the conserved CENP-C motif, an AT hook, and RK clusters (clusters enriched for arginine-lysine residues). Human CENP-C has two related DHBDs that bind preferentially to DNA sequences of higher AT content. Our findings suggest that a DNA composition-based mechanism together with residues characteristic for the CENP-A histone variant contribute to the specification of centromere identity.

SUBMITTER: Xiao H 

PROVIDER: S-EPMC5710141 | biostudies-literature | 2017 Oct

REPOSITORIES: biostudies-literature

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Molecular basis of CENP-C association with the CENP-A nucleosome at yeast centromeres.

Xiao Hua H   Wang Feng F   Wisniewski Jan J   Shaytan Alexey K AK   Ghirlando Rodolfo R   FitzGerald Peter C PC   Huang Yingzi Y   Wei Debbie D   Li Shipeng S   Landsman David D   Panchenko Anna R AR   Wu Carl C  

Genes & development 20171026 19


Histone CENP-A-containing nucleosomes play an important role in nucleating kinetochores at centromeres for chromosome segregation. However, the molecular mechanisms by which CENP-A nucleosomes engage with kinetochore proteins are not well understood. Here, we report the finding of a new function for the budding yeast Cse4/CENP-A histone-fold domain interacting with inner kinetochore protein Mif2/CENP-C. Strikingly, we also discovered that AT-rich centromere DNA has an important role for Mif2 rec  ...[more]

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