Hap2-Ino80-facilitated transcription promotes de novo establishment of CENP-A chromatin
Centromeres are maintained epigenetically by the presence of CENP-A, an evolutionarily conserved histone H3 variant, which directs kinetochore assembly and hence centromere function. To identify factors that promote assembly of CENP-A chromatin, we affinity-selected solubilized fission yeast CENP-A...
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Veröffentlicht in: | Genes & development 2020-02, Vol.34 (3-4), p.226-238 |
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Sprache: | eng |
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Zusammenfassung: | Centromeres are maintained epigenetically by the presence of CENP-A, an evolutionarily conserved histone H3 variant, which directs kinetochore assembly and hence centromere function. To identify factors that promote assembly of CENP-A chromatin, we affinity-selected solubilized fission yeast CENP-A
chromatin. All subunits of the Ino80 complex were enriched, including the auxiliary subunit Hap2. Chromatin association of Hap2 is Ies4-dependent. In addition to a role in maintenance of CENP-A
chromatin integrity at endogenous centromeres, Hap2 is required for de novo assembly of CENP-A
chromatin on naïve centromere DNA and promotes H3 turnover on centromere regions and other loci prone to CENP-A
deposition. Prior to CENP-A
chromatin assembly, Hap2 facilitates transcription from centromere DNA. These analyses suggest that Hap2-Ino80 destabilizes H3 nucleosomes on centromere DNA through transcription-coupled histone H3 turnover, driving the replacement of resident H3 nucleosomes with CENP-A
nucleosomes. These inherent properties define centromere DNA by directing a program that mediates CENP-A
assembly on appropriate sequences. |
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ISSN: | 0890-9369 1549-5477 |
DOI: | 10.1101/gad.332536.119 |