Chromatin Assembly at Kinetochores Is Uncoupled from DNA Replication

doi:10.1083/jcb.151.5.1113

Published online 20 November 2000. doi:10.1083/jcb.151.5.1113

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© The Rockefeller University Press, 0021-9525/2000/11/1113/ $5.00
The Journal of Cell Biology, Volume 151, Number 5, November 27, 2000 1113-1118

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Chromatin Assembly at Kinetochores Is Uncoupled from DNA Replication

Richard D. Shelby^a, Karine Monier^a, and Kevin F. Sullivan^a
^a Department of Cell Biology, The Scripps Research Institute, La Jolla, California 92037

Correspondence to: Kevin F. Sullivan, Department of Cell Biology MB38, The Scripps Research Institute, La Jolla, CA 92037. Tel:(858) 784-2350 Fax:(858) 784-2394

The specification of metazoan centromeres does not depend strictlyon centromeric DNA sequences, but also requires epigenetic factors.The mechanistic basis for establishing a centromeric "state"on the DNA remains unclear. In this work, we have directly examinedreplication timing of the prekinetochore domain of human chromosomes.Kinetochores were labeled by expression of epitope-tagged CENP-A,which stably marks prekinetochore domains in human cells. Byimmunoprecipitating CENP-A mononucleosomes from synchronizedcells pulsed with [³H]thymidine we demonstrate that CENP-A–associatedDNA is replicated in mid-to-late S phase. Cytological analysisof DNA replication further demonstrated that centromeres replicateasynchronously in parallel with numerous other genomic regions.In contrast, quantitative Western blot analysis demonstratesthat CENP-A protein synthesis occurs later, in G2. Quantitativefluorescence microscopy and transient transfection in the presenceof aphidicolin, an inhibitor of DNA replication, show that CENP-Acan assemble into centromeres in the absence of DNA replication.Thus, unlike most genomic chromatin, histone synthesis and assemblyare uncoupled from DNA replication at the kinetochore. UncouplingDNA replication from CENP-A synthesis suggests that regulatedchromatin assembly or remodeling could play a role in epigeneticcentromere propagation.

Key Words: kinetochore, centromere, chromatin, DNA replication, CENP-A

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