The spindle assembly checkpoint is a therapeutic vulnerability of CDK4/6 inhibitor–resistant ER
            <sup>+</sup>
            breast cancer with mitotic aberrations

Soria‐Bretones, Isabel; Thu, Kelsie L.; Silvester, Jennifer; Cruickshank, Jennifer; Ghamrasni, Samah El; Ba-Alawi, Wail; Fletcher, Graham C.; Kiarash, Reza; Elliott, Mitchell J.; Chalmers, Jordan J.; Elia, Andrea C.; Cheng, Amy; Rose, April A.N.; Bray, Mark R.; Haibe‐Kains, Benjamin; Mak, Tak W.; Cescon, David W.

doi:10.1126/sciadv.abq4293

Cited by 20 publications

(15 citation statements)

References 73 publications

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“…Likewise, for CAMA-1, copy number aberrations detected within cf-chromatin were largely concordant with those from nuclear WGS (Supplementary Fig. S2B) 78 . Furthermore, these copy number profiles were consistent across MNase digestion times (Supplementary Fig.…”

Section: Resultssupporting

confidence: 64%

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

De Michino,

Main,

Penny

et al. 2023

Preprint

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Cell-free chromatin (cf-chromatin) is a rich source of biomarkers across various conditions, including cancer. Tumor-derived circulating cf-chromatin can be profiled for epigenetic features, including nucleosome positioning and histone modifications that govern cell type-specific chromatin conformations. However, the low fractional abundance of tumor-derived cf-chromatin in blood and constrained access to plasma samples pose challenges for epigenetic biomarker discovery. Conditioned media from preclinical tissue culture models could provide an unencumbered source of pure tumor-derived cf-chromatin, but large cf-chromatin complexes from such models do not resemble the nucleosomal structures found predominantly in plasma, thereby limiting the applicability of many analysis techniques. Here, we developed a robust and generalizable framework for simulating cf-chromatin with physiologic nucleosomal distributions using an optimized nuclease treatment. We profiled the resulting nucleosomes by whole genome sequencing and confirmed that inferred nucleosome positioning reflected gene expression and chromatin accessibility patterns specific to the cell type. Compared with plasma, simulated cf-chromatin displayed stronger nucleosome positioning patterns at genomic locations of accessible chromatin from patient tissue. We then utilized simulated cf-chromatin to develop methods for genome-wide profiling of histone post-translational modifications associated with heterochromatin states. Cell-free chromatin immunoprecipitation and sequencing (cf-ChIP-Seq) of H3K27me3 identified heterochromatin domains associated with repressed gene expression, and when combined with H3K4me3 cfChIP-Seq revealed bivalent domains consistent with an intermediate state of transcriptional activity. Combining cfChIP-Seq of both modifications provided more accurate predictions of transcriptional activity from the cell of origin. Altogether, our results demonstrate the broad applicability of preclinical simulated cf-chromatin for epigenetic liquid biopsy biomarker discovery.

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Section: Resultssupporting

confidence: 64%

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

De Michino,

Main,

Penny

et al. 2023

Preprint

Self Cite

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“…In preclinical models of BC, the blockade of AURKA with its ATP‐competitive inhibitor alisertib induced mitotic spindle defects, mitotic delays and apoptosis, and displayed synergistic effects with the addition of paclitaxel 152–154 . Furthermore, our group recently showed the enhanced sensitivity to AURKAi alisertib, barasertib and tozasertib, of a panel of palbociclib‐resistant BC cells, characterised by an increased incidence of micronuclei and segregation errors 155 …”

Section: G2/m Phase Transitionmentioning

confidence: 93%

“…Another orally active TTKi, CFI‐402257, has shown preclinical monotherapy and taxane‐combination activity in HR + /HER2 − and TNBC models 184,192,193 . Of note, enhanced cytotoxicity has been observed in a subset of CDK4/6i‐resistant models, including those harbouring loss of RB1 155,184,193 . Currently, two phase 1/2 trials are underway evaluating CFI‐402257 in advanced solid tumours and BC.…”

Section: Mitotic Progressionmentioning

confidence: 99%

Seize the engine: Emerging cell cycle targets in breast cancer

Fuentes‐Antrás,

Bedard,

Cescon

2024

Clinical & Translational Med

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Breast cancer arises from a series of molecular alterations that disrupt cell cycle checkpoints, leading to aberrant cell proliferation and genomic instability. Targeted pharmacological inhibition of cell cycle regulators has long been considered a promising anti‐cancer strategy. Initial attempts to drug critical cell cycle drivers were hampered by poor selectivity, modest efficacy and haematological toxicity. Advances in our understanding of the molecular basis of cell cycle disruption and the mechanisms of resistance to CDK4/6 inhibitors have reignited interest in blocking specific components of the cell cycle machinery, such as CDK2, CDK4, CDK7, PLK4, WEE1, PKMYT1, AURKA and TTK. These targets play critical roles in regulating quiescence, DNA replication and chromosome segregation. Extensive preclinical data support their potential to overcome CDK4/6 inhibitor resistance, induce synthetic lethality or sensitise tumours to immune checkpoint inhibitors. This review provides a biological and drug development perspective on emerging cell cycle targets and novel inhibitors, many of which exhibit favourable safety profiles and promising activity in clinical trials.

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“…Although acquisition of RB1 loss on CDK4/6i is relatively rare in an unselected population, our results demonstrate that RB1 loss under the therapeutic pressure of CDK4/6i is observed almost exclusively in cancers who had only one functional allele of RB1 pretreatment. This has major clinical implications for advanced surveillance strategies and patient selection for clinical trials of precision therapeutic strategies directed against complete RB1 loss 50,51 . Most broadly, these results demonstrate how pre-treatment allelic structure of tumor suppressor genes may predict not only the therapeutic outcome of a particular targeted therapy, but may also forecast the specific mechanism by which a desired therapy will ultimately fail.…”

Section: Mainmentioning

confidence: 99%

Tumor suppressor heterozygosity and homologous recombination deficiency mediate resistance to front-line therapy in breast cancer

Safonov,

Marra,

Bandlamudi

et al. 2024

Preprint

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Germline and somatic variants that drive breast tumorigenesis and therapeutic sensitivity are widely prevalent. The clinical and biologic significance of co-occurring disease-defining germline and somatic events have yet to be defined and exploited. Using multiple, independent clinical cohorts comprising over 4500 patients, we identify that pathogenicRB1variants are enriched in gBRCA2-associated cancers, and manifest poor outcomes on standard-of-care front-line CDK4/6i plus antiestrogen combinations. We demonstrate gBRCA2-associated cancers commonly give rise to allelic configurations manifestingRB1heterozygosity and readily lose the second copy throughgBRCA2loss-mediated homologous recombination deficiency (HRD) under the therapeutic pressure of CDK4/6i. The findings unveil a novel therapeutic strategy of targeting the underlying HRD through PARPiprior toCDK4/6i to intercept the deleteriousRB1-loss trajectory. The work reveals how germline-somatic driven genomic configurations can shape treatment responses and be exploited in biomarker-directed clinical strategies.

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The spindle assembly checkpoint is a therapeutic vulnerability of CDK4/6 inhibitor–resistant ER ⁺ breast cancer with mitotic aberrations

Cited by 20 publications

References 73 publications

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

Seize the engine: Emerging cell cycle targets in breast cancer

Tumor suppressor heterozygosity and homologous recombination deficiency mediate resistance to front-line therapy in breast cancer

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The spindle assembly checkpoint is a therapeutic vulnerability of CDK4/6 inhibitor–resistant ER + breast cancer with mitotic aberrations

Cited by 20 publications

References 73 publications

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

Simulating cell-free chromatin using preclinical models for cancer-specific biomarker discovery

Seize the engine: Emerging cell cycle targets in breast cancer

Tumor suppressor heterozygosity and homologous recombination deficiency mediate resistance to front-line therapy in breast cancer

Contact Info

Product

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The spindle assembly checkpoint is a therapeutic vulnerability of CDK4/6 inhibitor–resistant ER ⁺ breast cancer with mitotic aberrations