The presence of extra chromosomes leads to genomic instability

Publication date

2016-02-15

Authors

Passerini, Verena
Ozeri-Galai, Efrat
De Pagter, Mirjam S.
Donnelly, Neysan
Schmalbrock, Sarah
Kloosterman, Wigard P.ISNI 0000000390600212
Kerem, Batsheva
Storchová, Zuzana

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Abstract

Aneuploidy is a hallmark of cancer and underlies genetic disorders characterized by severe developmental defects, yet the molecular mechanisms explaining its effects on cellular physiology remain elusive. Here we show, using a series of human cells with defined aneuploid karyotypes, that gain of a single chromosome increases genomic instability. Next-generation sequencing and SNP-array analysis reveal accumulation of chromosomal rearrangements in aneuploids, with break point junction patterns suggestive of replication defects. Trisomic and tetrasomic cells also show increased DNA damage and sensitivity to replication stress. Strikingly, we find that aneuploidy-induced genomic instability can be explained by the reduced expression of the replicative helicase MCM2-7. Accordingly, restoring near-wild-type levels of chromatin-bound MCM helicase partly rescues the genomic instability phenotypes. Thus, gain of chromosomes triggers replication stress, thereby promoting genomic instability and possibly contributing to tumorigenesis.

Keywords

General Biochemistry,Genetics and Molecular Biology, General Chemistry, General Physics and Astronomy, Journal Article, Research Support, Non-U.S. Gov't

Citation

Passerini, V, Ozeri-Galai, E, De Pagter, M S, Donnelly, N, Schmalbrock, S, Kloosterman, W P, Kerem, B & Storchová, Z 2016, 'The presence of extra chromosomes leads to genomic instability', Nature Communications [E], vol. 7, 10754. https://doi.org/10.1038/ncomms10754