Abstract

Chromosomal instability (CIN) is a hallmark of many cancers and a major contributor to tumorigenesis. Centromere and kinetochore associated proteins such as the evolutionarily conserved centromeric histone H3 variant CENP-A, associate with centromeric DNA for centromere function and chromosomal stability. Stringent regulation of cellular CENP-A levels prevents its mislocalization in yeast and flies to maintain genome stability. CENP-A overexpression and mislocalization are observed in several cancers and reported to be associated with increased invasiveness and poor prognosis. We examined whether there is a direct relationship between mislocalization of overexpressed CENP-A and CIN using HeLa and chromosomally stable diploid RPE1 cell lines as model systems. Our results show that mislocalization of overexpressed CENP-A to chromosome arms leads to chromosome congression defects, lagging chromosomes, micronuclei formation and a delay in mitotic exit. CENP-A overexpressing cells showed altered localization of centromere and kinetochore associated proteins such as CENP-C, CENP-T and Nuf2 leading to weakened native kinetochores as shown by reduced interkinetochore distance and CIN. Importantly, our results show that mislocalization of CENP-A to chromosome arms is one of the major contributors for CIN as depletion of histone chaperone DAXX prevents CENP-A mislocalization and rescues the reduced interkinetochore distance and CIN phenotype in CENP-A overexpressing cells. In summary, our results establish that CENP-A overexpression and mislocalization result in a CIN phenotype in human cells. This study provides insights into how overexpression of CENP-A may contribute to CIN in cancers and underscore the importance of understanding the pathways that prevent CENP-A mislocalization for genome stability.

Highlights

  • Chromosomal instability (CIN), a hallmark of aggressive tumors and birth defects, is characterized by unequal distribution of chromosomes into two daughter cells and/or structural rearrangements of the genome

  • Our results show a dose-dependent effect of CENP-A overexpression on chromosome segregation defects and higher incidence of micronuclei

  • We show that mislocalization of CENP-A is the major contributor for a CIN phenotype as preventing mislocalization of CENP-A to chromosome arms suppresses CENP-A overexpression induced chromosome segregation defects

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Summary

Introduction

Chromosomal instability (CIN), a hallmark of aggressive tumors and birth defects, is characterized by unequal distribution of chromosomes into two daughter cells (numerical CIN) and/or structural rearrangements of the genome (structural CIN). Numerical CIN is often caused by chromosome segregation errors due to mitotic abnormalities such as defective sister chromatid cohesion, over duplication of centrosomes, erroneous kinetochoremicrotubule attachments and deregulation of spindle assembly checkpoint (SAC) [4]. One of the key determinants for chromosomal stability is the centromere which serves as a site for kinetochore assembly and a locus for kinetochoremicrotubule (KT-MT) attachments and SAC functions. CCAN (Constitutive Centromere Associated Network) proteins such as CENP-C and CENP-N associate with CENP-A, whereas CENP-T and CENP-W associate with histone H3 nucleosomes [8,9,10]. CCAN proteins and the CENP-A nucleosome provide a platform for assembling the kinetochore and associated proteins for efficient KT-MT attachment and faithful chromosome segregation [14,15,16]

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