Hyperactivation of MAPK Induces Tamoxifen Resistance in SPRED2-Deficient ERα-Positive Breast Cancer

Vafeiadou, Vasiliki; Hany, Dina; Picard, Didier

doi:10.3390/cancers14040954

Cited by 15 publications

(12 citation statements)

References 86 publications

(105 reference statements)

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“…1, B and C). We have recently shown that SPRED2 deficiency is an important indicator of tamoxifen resistance because of ERα hyperactivation through the MAPK signaling pathway ( 37 ).…”

Section: Resultsmentioning

confidence: 99%

CRISPR/Cas9 screen reveals a role of purine synthesis for estrogen receptor α activity and tamoxifen resistance of breast cancer cells

Hany

Vafeiadou

Picard

2022

Preprint

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In breast cancer, resistance to endocrine therapies that target estrogen receptor α (ERα), such as tamoxifen and fulvestrant, remains a major clinical problem. Whether and how ERα+ breast cancers switch from being estrogen-dependent to -independent remains unclear. With a genome-wide CRISPR/Cas9 knockout screen, we identified new biomarkers and potential therapeutic targets of endocrine resistance. We demonstrate that high levels of PAICS, an enzyme involved in the de novo biosynthesis of purines, can shift the balance of ERα activity to be more estrogen-independent and tamoxifen-resistant. We indicate that this is due to an elevated activity of cAMP-activated protein kinase A and mammalian target of rapamycin, kinases known to phosphorylate ERα specifically and to stimulate its activity. Genetic or pharmacological targeting of PAICS sensitizes tamoxifen-resistant cells to tamoxifen. Based on these findings, we propose the combined targeting of PAICS and ERα as a new, effective, and potentially safe therapeutic regimen.

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“…1, B and C). We have recently shown that SPRED2 deficiency is an important indicator of tamoxifen resistance because of ERα hyperactivation through the MAPK signaling pathway ( 37 ).…”

Section: Resultsmentioning

confidence: 99%

CRISPR/Cas9 screen reveals a role of purine synthesis for estrogen receptor α activity and tamoxifen resistance of breast cancer cells

Hany

Vafeiadou

Picard

2022

Preprint

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“…The approach is based on a phenotypic assay of the cellular ATP levels, which reflect the metabolic activity, and hence, the viability of cells. We initially screened drug combinations using the three ERα+ breast cancer cell lines, MCF7 (tamoxifen-sensitive), MCF7-V (a more tamoxifen-tolerant variant of MCF7) (Vafeiadou et al , 2022; Mohammadi Ghahhari et al , 2022), and MCF7/LCC2 (tamoxifen-resistant) (Brünner et al , 1993). In parallel, we used MCF10A, a non-malignant breast epithelial cell line, to monitor the relative toxicity, and to calculate the therapeutic window (TW), which represents the difference in efficacy between cancerous and non-cancerous cells.…”

Section: Resultsmentioning

confidence: 99%

“…In addition, ERα can be activated in an estrogen- independent manner by a large panel of factors, including epidermal growth factor (EGF) (Ignar-Trowbridge et al , 1992; Ignar-Trowbridge et al , 1993), insulin and insulin-like growth factors (IGF) (Newton et al , 1994), PI3K (Campbell et al , 2001), Akt (Campbell et al , 2001; Martin et al , 2000), and hypoxia-inducible factor 1 α (HIF1α) (Cho et al , 2006; Bennesch & Picard, 2015) (see detailed list at https://www.picard.ch/downloads/Factors.pdf). Through various domains, ERα can interact with a plethora of proteins that regulate its activity, such as the MAPKs ERK1/ERK2 (ERK1/2) (Chen et al , 2002; Kato et al , 1995; Kim et al , 2021; Vafeiadou et al , 2022; Li et al , 2012; Mueller et al , 2000; Bunone et al , 1996), mTOR (Alayev et al , 2016), cyclin-dependent kinase inhibitor 1 (p21) (Fritah et al , 2005; Redeuilh et al , 2002; Abukhdeir et al , 2008), and poly (ADP-ribose) polymerase 1 (PARP1) (Schiewer & Knudsen, 2014; Zhang et al , 2013; Pulliam et al , 2019; Gadad et al , 2021) (see the updated list of ERα interactors at https://www.picard.ch/downloads).…”

Section: Introductionmentioning

confidence: 99%

“…Resistance to tamoxifen can be attributed to multiple mechanisms, including loss of ERα expression or function due to genetic mutations, alterations in the levels of co-regulatory factors (Osborne et al , 2003), upregulation of oncogenic signal transduction pathways, and ligand-independent activation of ERα (Kato et al , 1995; Shim et al , 2000; Coutts & Murphy, 1998; Gee et al , 2001; Clark et al , 2002; Gutierrez et al , 2005; Bennesch & Picard, 2015). For example, ERK1/2 play a critical role in breast cancer and their hyperactivation is associated with tamoxifen resistance and poor prognosis (Gee et al , 2001; Coutts & Murphy, 1998; Shim et al , 2000; Chen et al , 2002; Kato et al , 1995; Kim et al , 2021; Vafeiadou et al , 2022; Li et al , 2012; Mueller et al , 2000; Bunone et al , 1996). ERK1/2 can stimulate cell growth independently of ERα or through signaling crosstalk with ERα.…”

Section: Introductionmentioning

confidence: 99%

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Network-informed discovery of multidrug combinations for ERα+/HER2-/PI3Kα-mutant breast cancer

Hany

Zoetemelk

Bhattacharya

et al. 2022

Preprint

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Breast cancer is a persistent threat to women worldwide. A large proportion of breast cancers are dependent on estrogen receptor α (ERα) for tumor progression. Therefore, targeting ERα with antagonists, such as tamoxifen, remains standard therapy for ERα+ breast cancer. The clinical benefits of monotherapy are often counterbalanced by off-target toxicity and development of resistance. Combinations of more than two drugs might be of great therapeutic value to prevent resistance, and to reduce doses, and hence, toxicity. We mined data from the literature and public repositories to construct a network of potential drug targets for synergistic multidrug combinations. With 9 drugs, we performed a phenotypic combinatorial screen with ERα+ breast cancer cell lines. We identified two optimized low-dose combinations of 3 and 4 drugs of high therapeutic relevance to the frequent ERα+/HER2-/PI3Kα-mutant subtype of breast cancer. Moreover, we validated the efficacy of the combinations in tamoxifen-resistant cell lines, patient-derived organoids, and xenograft experiments. Thus, we propose multidrug combinations that have the potential to overcome the standard issues of current monotherapies.

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“…NF1-knockout MCF7 cells showed increased levels of phospho-ERK and resistance to fulvestrant, which could be reverted by ERK inhibitors [ 85 ]. Similarly, downregulation of Sprouty-related EVH1 domain containing 2 (SPRED2), a member of the Sprouty family of RAS inhibitors, frequently altered in breast cancer due to deletion or promoter methylation, leads to tamoxifen resistance, which can be overcome in breast cancer cell lines by a combination of the ERK 1/2 inhibitor ulixertinib with tamoxifen [ 112 ]. RAS mutations have been identified in circulating tumor DNA in 15% of patients who had disease progression under aromatase inhibitors, potentially mediating resistance [ 113 ].…”

Section: Ras/raf/mek/erk Pathway In Luminal Cancers and Resistance To...mentioning

confidence: 99%

The Predictive and Prognostic Role of RAS–RAF–MEK–ERK Pathway Alterations in Breast Cancer: Revision of the Literature and Comparison with the Analysis of Cancer Genomic Datasets

Rocca

Braga

Volpe

et al. 2022

Cancers

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Although gene alterations of the RAS/RAF/MEK/ERK pathway are uncommon in breast cancer, this pathway is frequently activated in breast tumors, implying its role in tumor progression. We describe, after a revision of the literature, the frequency and types of gene alterations affecting this pathway in breast cancer by analyzing some public datasets from cBioPortal. Moreover, we consider their prognostic and predictive impact on treatment response, along with the role of transcriptomic predictors of RAS pathway activation. Our analysis shows that the driver alterations in RAS/RAF/MEK/ERK pathway-related genes are detected in 11% of primary breast cancers. The most frequently mutated genes are NF1 and KRAS, while copy number alterations mainly affect KRAS and BRAF, especially in basal-like tumors. The subgroup of patients carrying these alterations shows a worse prognosis; alterations in NF1 and RAF1 are associated with significantly reduced breast-cancer-specific survival in multivariate analysis. The literature review shows that the pathway is implicated, either by genetic or epigenetic alterations or by signaling network adaptations, in the mechanisms of sensitivity and resistance to a wide range of drugs used in the treatment of breast cancer. A thorough understanding of these alterations is critical for developing combination therapies that can delay or overcome drug resistance.

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Hyperactivation of MAPK Induces Tamoxifen Resistance in SPRED2-Deficient ERα-Positive Breast Cancer

Cited by 15 publications

References 86 publications

CRISPR/Cas9 screen reveals a role of purine synthesis for estrogen receptor α activity and tamoxifen resistance of breast cancer cells

CRISPR/Cas9 screen reveals a role of purine synthesis for estrogen receptor α activity and tamoxifen resistance of breast cancer cells

Network-informed discovery of multidrug combinations for ERα+/HER2-/PI3Kα-mutant breast cancer

The Predictive and Prognostic Role of RAS–RAF–MEK–ERK Pathway Alterations in Breast Cancer: Revision of the Literature and Comparison with the Analysis of Cancer Genomic Datasets

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