Assembly Principles and Stoichiometry of a Complete Human Kinetochore Module

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2021 Jul 1

PMID 34193424

Citations 25

Authors

Kai Walstein

Arsen Petrovic

Dongqing Pan

Birte Hagemeier

Dorothee Vogt

Ingrid R Vetter

Andrea Musacchio

Affiliations

Soon will be listed here.

Abstract

Centromeres are epigenetically determined chromosomal loci that seed kinetochore assembly to promote chromosome segregation during cell division. CENP-A, a centromere-specific histone H3 variant, establishes the foundations for centromere epigenetic memory and kinetochore assembly. It recruits the constitutive centromere-associated network (CCAN), which in turn assembles the microtubule-binding interface. How the specific organization of centromeric chromatin relates to kinetochore assembly and to centromere identity through cell division remains conjectural. Here, we break new ground by reconstituting a functional full-length version of CENP-C, the largest human CCAN subunit and a blueprint of kinetochore assembly. We show that full-length CENP-C, a dimer, binds stably to two nucleosomes and permits further assembly of all other kinetochore subunits in vitro with relative ratios closely matching those of endogenous human kinetochores. Our results imply that human kinetochores emerge from clustering multiple copies of a fundamental module and may have important implications for transgenerational inheritance of centromeric chromatin.

Citing Articles

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