Near‐tetraploid cancer cells show chromosome instability triggered by replication stress and exhibit enhanced invasiveness

Wangsa, Darawalee; Quintanilla, Isabel; Torabi, Keyvan; Vila-Casadesús, María; Ercilla, Amaia; Klus, Gregory T.; Yüce, Zeynep; Galofré, Claudia; Cuatrecasas, Míriam; Lozano, Juan José; Agell, Neus; Cimini, Daniela; Castells, Antoni; Ried, Thomas; Camps, Jordi

doi:10.1096/fj.201700247rr

Cited by 55 publications

(68 citation statements)

References 61 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…4d-e). These data reveal that WGD + tumor cells are more dependent on specific DNA replication factors relative to WGD − tumor cells, perhaps as a means to compensate for increased replication stress induced by tetraploidy 41,42 . These results are particularly significant in therapeutic contexts as gemcitabine and other inhibitors of ribonucleotide reductase represent the standard of care for treatment regimens across multiple cancer subtypes, and biomarkers that can predict sensitivity to gemcitabine hold real prognostic value 43 .…”

Section: Wgd Confers Unique Genetic Vulnerabilities On Tumorsmentioning

confidence: 83%

Whole genome doubling confers unique genetic vulnerabilities on tumor cells

Quinton

DiDomizio

Vittoria

et al. 2020

Preprint

View full text Add to dashboard Cite

47Whole genome doubling (WGD) occurs early in tumorigenesis and generates genetically 48 unstable tetraploid cells that fuel tumor development. Cells that undergo WGD (WGD + ) 49 must adapt to accommodate their abnormal tetraploid state; however, the nature of these 50 adaptations, and whether they confer vulnerabilities that can subsequently be exploited 51 therapeutically, is unclear. Using sequencing data from ~10,000 primary human cancer 52 samples and essentiality data from ~600 cancer cell lines, we show that WGD gives rise to 53 common genetic traits that are accompanied by unique vulnerabilities. We reveal that 54 WGD + cells are more dependent on spindle assembly checkpoint signaling, DNA 55 replication factors, and proteasome function than WGDcells. We also identify KIF18A, 56 which encodes for a mitotic kinesin, as being specifically required for the viability of 57 WGD + cells. While loss of KIF18A is largely dispensable for accurate chromosome 58 segregation during mitosis in WGDcells, its loss induces dramatic mitotic errors in 59 WGD + cells, ultimately impairing cell viability. Collectively, our results reveal new 60 strategies to specifically target WGD + cancer cells while sparing the normal, non-61 transformed WGDcells that comprise human tissue. 62The vast majority of human cells are diploid and numerous cell cycle controls exist to help 63 ensure that this state is maintained across successive cell divisions 1 . Despite these controls, 64 errors can occur that result in a whole genome doubling (WGD), in which a natively diploid cell 65 transitions to a tetraploid state 1-3 . It has been demonstrated that cells that have experienced a 66 WGD event (hereafter WGD + ) are oncogenic and can facilitate tumorigenesis 4,5 . WGD promotes 67 tumorigenesis in at least two ways: first, proliferating WGD + cells are genomically unstable and 68 rapidly accumulate both numerical and structural chromosomal abnormalities 5 , and second, 69 WGD + cells are better able to buffer against the negative effects of deleterious mutations and 70 ongoing chromosome instability 6-10 . Such traits enable nascent WGD + tumor cells to proliferate 71 in the presence of otherwise lethal genomic alterations while simultaneously sampling increased 72 genetic permutations, ultimately enabling phenotypic leaps that give rise to tumors 8,11 . WGD also 73 carries important clinical implications, with recent reports showing its correlation with advanced 74 metastatic disease and a worse overall prognosis 12,13 . 75 76 Given the oncogenic potential associated with WGD, tumor suppression mechanisms exist to limit 77 the proliferation of these unstable cells. WGD + cells activate both the p53 and Hippo tumor 78 suppressor pathways and are prone to apoptosis, senescence, and immune clearance [14][15][16] . WGD also 79gives rise to numerous abnormalities in cellular physiology that impair fitness 6,14,17 . Therefore, in 80 order to promote tumorigenesis, WGD + cells must adapt to overcome these barriers 5,14,18,19 . Thus, 81 while ...

show abstract

Section: Wgd Confers Unique Genetic Vulnerabilities On Tumorsmentioning

confidence: 83%

Whole genome doubling confers unique genetic vulnerabilities on tumor cells

Quinton

DiDomizio

Vittoria

et al. 2020

Preprint

View full text Add to dashboard Cite

show abstract

“…It has been posited that polyploid tumors with elevated genomic content tend to become resistant to chemotherapy due to rapid tumor evolution (49). In addition, neartetraploid cancer cells have recently been shown to exhibit enhanced invasiveness (50). It will be of interest to determine whether high ploidy status per se is able to contribute to SASPinduced tumor progression.…”

Section: Wwwaacrjournalsorgmentioning

confidence: 99%

Autophagy Governs Protumorigenic Effects of Mitotic Slippage–induced Senescence

Jakhar

Luijten

Wong

et al. 2018

Molecular Cancer Research

View full text Add to dashboard Cite

The most commonly utilized class of chemotherapeutic agents administered as a first-line therapy are antimitotic drugs; however, their clinical success is often impeded by chemoresistance and disease relapse. Hence, a better understanding of the cellular pathways underlying escape from cell death is critical. Mitotic slippage describes the cellular process where cells exit antimitotic drug-enforced mitotic arrest and "slip" into interphase without proper chromosome segregation and cytokinesis. The current report explores the cell fate consequence following mitotic slippage and assesses a major outcome following treatment with many chemotherapies, therapy-induced senescence. It was found that cells postslippage entered senescence and could impart the senescence-associated secretory phenotype (SASP). SASP factor production elicited paracrine protumorigenic effects, such as migration, invasion, and vascularization. Both senescence and SASP factor development were found to be dependent on autophagy. Autophagy induction during mitotic slippage involved the autophagy activator AMPK and endoplasmic reticulum stress response protein PERK. Pharmacologic inhibition of autophagy or silencing of autophagy-related ATG5 led to a bypass of G arrest senescence, reduced SASP-associated paracrine tumorigenic effects, and increased DNA damage after S-phase entry with a concomitant increase in apoptosis. Consistent with this, the autophagy inhibitor chloroquine and microtubule-stabilizing drug paclitaxel synergistically inhibited tumor growth in mice. Sensitivity to this combinatorial treatment was dependent on p53 status, an important factor to consider before treatment. Clinical regimens targeting senescence and SASP could provide a potential effective combinatorial strategy with antimitotic drugs. .

show abstract

“…23), supporting the potential role of polyploidy in tumour development. A recent study reported that near-tetraploid cancer cells exhibited elevated invasiveness and displayed CIN (215), lending support to our findings. Our results therefore describe another mechanism by which polyploidization per se has the potential to contribute to tumourigenesis through senescence and SASP.…”

Section: Potential Role Of Polyploidy In Senescence and Tumourigenesissupporting

confidence: 91%

“…Notably, we observed an enrichment of cells displaying 3 or more signals for these two chromosomes at the invasive fronts compared to cells in the centre region and the normal area, suggesting the existence of near-triploid and near-tetraploid cells at the invasive front. This finding is in line with a recent study that revealed the presence of near-tetraploid cancer cells at the invasive front in primary colorectal tumours, which led to their speculation that tetraploidy could promote the invasiveness and aggressiveness of cancer cells (215). Importantly, our study revealed a correlation of greater deviation from the diploidy with increased incidence of senescence and SASP at the invasion front, indicating that the pro-tumourgenic paracrine effects of SASP from senescent tumour cells might plausibly promote the aggressive behaviour of tumour cells at the invasive front, as described previously in vitro.…”

Section: Senescent and Aneuploid Cells Are Frequently Present At The supporting

confidence: 90%

Chromosomal instability-induced senescence potentiates cell non-autonomous tumourigenic effects

He¹

View full text Add to dashboard Cite

show abstract

Near‐tetraploid cancer cells show chromosome instability triggered by replication stress and exhibit enhanced invasiveness

Cited by 55 publications

References 61 publications

Whole genome doubling confers unique genetic vulnerabilities on tumor cells

Whole genome doubling confers unique genetic vulnerabilities on tumor cells

Autophagy Governs Protumorigenic Effects of Mitotic Slippage–induced Senescence

Chromosomal instability-induced senescence potentiates cell non-autonomous tumourigenic effects

Contact Info

Product

Resources

About