The centromere is the chromosomal locus that recruits the kinetochore, directing faithful propagation of the genome during cell division. Using cryo-ET on human mitotic chromosomes, we reveal a distinctive architecture at the centromere: clustered 20- to 25-nm nucleosome-associated complexes within chromatin clearings that delineate them from surrounding chromatin. Centromere components CENP-C and CENP-N are each required for the integrity of the complexes, while CENP-C is also required to maintain the chromatin clearing. We find that CENP-C is required in mitosis, not just for kinetochore assembly, likely reflecting its role in organizing the inner kinetochore during chromosome segregation. We further visualize the scaffold of the fibrous corona, a structure amplified at unattached kinetochores, revealing crescent-shaped parallel arrays of fibrils extending >1 μm. Thus, we reveal how the organization of centromeric chromatin creates a clearing at the site of kinetochore formation as well as the nature of kinetochore amplification mediated by corona fibrils.
Centromeric chromatin clearings demarcate the site of kinetochore formation.
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作者:Kixmoeller Kathryn, Tarasovetc Ekaterina V, Mer Elie, Chang Yi-Wei, Black Ben E
| 期刊: | Cell | 影响因子: | 42.500 |
| 时间: | 2025 | 起止号: | 2025 Mar 6; 188(5):1280-1296 |
| doi: | 10.1016/j.cell.2024.12.025 | ||
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