Whole-Genome Duplication and Genome Instability in Cancer Cells: Double the Trouble

Whole-genome duplication (WGD) is one of the most common genomic abnormalities in cancers. WGD can provide a source of redundant genes to buffer the deleterious effect of somatic alterations and facilitate clonal evolution in cancer cells. The extra DNA and centrosome burden after WGD is associated...

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Bibliographic Details
Published inInternational journal of molecular sciences Vol. 24; no. 4; p. 3733
Main Authors Lau, Tsz Yin, Poon, Randy Y C
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 01.02.2023
MDPI
Subjects
Abnormalities
Apoptosis
Cancer
Cancer cells
Carcinogenesis - genetics
Cell Cycle
centrosome
Centrosome - metabolism
Centrosomes
Chromosomal Instability
Chromosomes
Clustering
Cyclin-dependent kinases
Cytokinesis
Deoxyribonucleic acid
Diploids
DNA
DNA biosynthesis
DNA damage
Failure
Gene Duplication
Genetic aspects
genome instability
Genomes
Genomic Instability
Genomics
Health aspects
Humans
Kinases
kinesin
Mitosis
Neoplasms - genetics
p53 Protein
ploidy
Polyploidy
Replication
Reproduction (copying)
Review
Spindle Apparatus
Stability
Supernumerary
Tactics
tetraploidization
tetraploidization
genome instability
centrosome
mitosis
kinesin
ploidy
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Summary:Whole-genome duplication (WGD) is one of the most common genomic abnormalities in cancers. WGD can provide a source of redundant genes to buffer the deleterious effect of somatic alterations and facilitate clonal evolution in cancer cells. The extra DNA and centrosome burden after WGD is associated with an elevation of genome instability. Causes of genome instability are multifaceted and occur throughout the cell cycle. Among these are DNA damage caused by the abortive mitosis that initially triggers tetraploidization, replication stress and DNA damage associated with an enlarged genome, and chromosomal instability during the subsequent mitosis in the presence of extra centrosomes and altered spindle morphology. Here, we chronicle the events after WGD, from tetraploidization instigated by abortive mitosis including mitotic slippage and cytokinesis failure to the replication of the tetraploid genome, and finally, to the mitosis in the presence of supernumerary centrosomes. A recurring theme is the ability of some cancer cells to overcome the obstacles in place for preventing WGD. The underlying mechanisms range from the attenuation of the p53-dependent G checkpoint to enabling pseudobipolar spindle formation via the clustering of supernumerary centrosomes. These survival tactics and the resulting genome instability confer a subset of polyploid cancer cells proliferative advantage over their diploid counterparts and the development of therapeutic resistance.
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ISSN:1422-0067
1661-6596
1422-0067
DOI:10.3390/ijms24043733