4.2 Article

The role of CENP-B and alpha-satellite DNA: de novo assembly and epigenetic maintenance of human centromeres

Journal

CHROMOSOME RESEARCH
Volume 12, Issue 6, Pages 543-556

Publisher

KLUWER ACADEMIC PUBL
DOI: 10.1023/B:CHRO.0000036593.72788.99

Keywords

alphoid DNA; CENP-A; CENP-B; centromere; epigenetics; human artificial chromosome

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The centromere is an essential functional domain responsible for the correct inheritance of eukaryotic chromosomes during cell division. Eukaryotic centromeres include the highly conserved centromere-specific histone H3 variant, CENP-A, which has provided a powerful tool for investigating the recruitment of centromere components. However, the trigger that targets CENP-A to a specific genomic locus during centromere assembly remains unknown. Although, on rare occasions, CENP-A chromatin may assemble at non-centromeric DNA, all normal human centromeres are assembled and maintained on alpha-satellite (alphoid) DNA. The importance of alphoid DNA and CENP-B binding sites (CENP-B boxes), typical of normal human centromere DNA configurations, has been demonstrated through their requirement in de novo centromere assembly and Human Artificial Chromosome ( HAC) assays. Mechanisms to link the centromere tightly to specific genomic sequences exist in humans and the two yeast species.

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