1. Both tails and the centromere targeting domain of CENP-A are required for centromere establishment
- Author
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Lucie Y. Guo, Jamie E. DeNizio, Jennine M. Dawicki-McKenna, Ben E. Black, Evelyne J. Barrey, Glennis A. Logsdon, Emily A. Bassett, Tanya Panchenko, and Patrick Heun
- Subjects
Cell division ,Chromosomal Proteins, Non-Histone ,Centromere ,lac operon ,macromolecular substances ,Biology ,Lac repressor ,Autoantigens ,Histones ,03 medical and health sciences ,Histone H3 ,0302 clinical medicine ,Report ,Cell Line, Tumor ,Centromere Protein A ,Humans ,Nucleosome ,Research Articles ,030304 developmental biology ,Genetics ,0303 health sciences ,Cell Biology ,Protein Structure, Tertiary ,3. Good health ,Histone ,biology.protein ,030217 neurology & neurosurgery - Abstract
New roles for the N-terminal histone tail and folded core of CENP-A are revealed by monitoring early steps in centromere establishment., The centromere—defined by the presence of nucleosomes containing the histone H3 variant, CENP-A—is the chromosomal locus required for the accurate segregation of chromosomes during cell division. Although the sequence determinants of human CENP-A required to maintain a centromere were reported, those that are required for early steps in establishing a new centromere are unknown. In this paper, we used gain-of-function histone H3 chimeras containing various regions unique to CENP-A to investigate early events in centromere establishment. We targeted histone H3 chimeras to chromosomally integrated Lac operator sequences by fusing each of the chimeras to the Lac repressor. Using this approach, we found surprising contributions from a small portion of the N-terminal tail and the CENP-A targeting domain in the initial recruitment of two essential constitutive centromere proteins, CENP-C and CENP-T. Our results indicate that the regions of CENP-A required for early events in centromere establishment differ from those that are required for maintaining centromere identity.
- Published
- 2015
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