Effect of selumetinib on the growth of anastrozole-resistant tumors

Sabnis, Gauri; Kazi, Armina A.; Golubeva, O.; Shah, Preeti; Brodie, Angela

doi:10.1007/s10549-013-2474-5

Cited by 12 publications

(10 citation statements)

References 41 publications

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“…Thus, combinatorial treatment blocking both ER and growth factor signaling pathways has been suggested to be the most effective inhibition of proliferation in ER positive breast cancer cells [12,16,51,53,54]. In line with this, treatment with the MAPK/ERK kinase inhibitor, selumetinib reversed the AI resistance in mice exhibiting anastrozole resistant tumors [55]. Adding the dual EGFR/HER-1 / HER-2/neu inhibitor lapatinib to the AI inhibitor letrozole improved the progression free survival (PFS) in patients with ER positive/HER-2/neu amplified tumors, whereas no effects were observed in the ER positive/HER-2/neu non-amplified subgroup [56].…”

Section: Treatment With Ais For 3-4 Months Suppresses Total Body Estrmentioning

confidence: 89%

Treatment with aromatase inhibitors stimulates the expression of epidermal growth factor receptor-1 and neuregulin 1 in ER positive/HER-2/neu non-amplified primary breast cancers

Flågeng

Larionov

Geisler

et al. 2017

The Journal of Steroid Biochemistry and Molecular Biology

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While estrogens have been shown to modulate EGFR/HER-1 and HER-2/neu expression in experimental systems, the effects of estrogen deprivation on expression levels of the HER-receptors and the neuregulin (NRG)1 ligand in breast cancers remain unknown. Here, we measured EGFR/HER-1-4 and NRG1 mRNA in ER positive tumors from 85 postmenopausal breast cancer patients before and after two weeks (n=64) and three months (n=85) of primary treatment with an aromatase inhibitor (AI). In tumors lacking HER-2/neu amplification, quantitative real-time PCR analyses revealed EGFR/HER-1 and NRG1 to vary significantly between the three time points (before therapy, after 2 weeks and after 3 months on treatment; P≤0.001 for both). Pair-wise comparison revealed a significant increase in EGFR/HER-1 already during the first two weeks of treatment (P=0.049) with a further increase for both EGFR/HER-1 and NRG1 after 3 months on treatment (P≤0.001 and P=0.001 for both comparing values at 3 months to values at baseline and 2 weeks respectively). No difference between tumors responding versus non-responders was recorded. Further, no significant change in any parameter was observed among HER-2/neu amplified tumors. Analyzing components of the HER-2/neu PI3K/Akt downstream pathway, the PIK3CA H1047R mutation was associated with treatment response (P=0.035); however no association between either AKT phosphorylation status or PIK3CA gene mutations and EGFR/HER-1 or NRG1 expression levels were observed. Our results indicate primary AI treatment to modulate expression of HER-family members and the growth factor NRG1 in HER-2/neu non-amplified breast cancers in vivo. Potential implications to long term sensitivity warrants further investigations.

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Section: Treatment With Ais For 3-4 Months Suppresses Total Body Estrmentioning

confidence: 89%

Treatment with aromatase inhibitors stimulates the expression of epidermal growth factor receptor-1 and neuregulin 1 in ER positive/HER-2/neu non-amplified primary breast cancers

Flågeng

Larionov

Geisler

et al. 2017

The Journal of Steroid Biochemistry and Molecular Biology

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“…The lack of frequent mutations within the core Ras-Raf-MEK axis, but the potential for cross-talk with a plethora of pathways intrinsic to breast cancer progression, may mean that the potential of MEK blockade lies in treatment combinations to overcome resistance. This is borne out by pre-clinical studies which have shown MEK inhibition has the potential to enhance sensitivity of breast cancer xenografts to HER2 blockade [ 105 ] and anti-estrogen treatment [ 106 ]. Furthermore, studies with breast cancer cell lines have shown that MEK inhibition also increases sensitivity to EGFR blockade [ 107 ], and reversed the effects of IGF-1R overexpression in promoting proliferation [ 108 ].…”

Section: Discussionmentioning

confidence: 99%

Stimulus-dependent differences in signalling regulate epithelial-mesenchymal plasticity and change the effects of drugs in breast cancer cell lines

et al. 2015

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Introduction: The normal process of epithelial mesenchymal transition (EMT) is subverted by carcinoma cells to facilitate metastatic spread. Cancer cells rarely undergo a full conversion to the mesenchymal phenotype, and instead adopt positions along the epithelial-mesenchymal axis, a propensity we refer to as epithelial mesenchymal plasticity (EMP). EMP is associated with increased risk of metastasis in breast cancer and consequent poor prognosis. Drivers towards the mesenchymal state in malignant cells include growth factor stimulation or exposure to hypoxic conditions.

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“…As demonstrated previously, ectopic overexpression of HER2 in human breast cancer cells correlates with increases in TIC characteristics, including mammosphere formation, expression of the breast cancer resistance protein (BCRP), and side population (SP)-positive cells [5]. AI-resistant cell lines, including LTLT-Ca and Ac1ANAR (anastrozole resistant, [6]), have increased HER2 expression when compared to their parental controls, which is accompanied by increased expression of TIC characteristics [5,7]. Furthermore, lapatinib treatment reduced SP and mammosphere formation [7] in LTLT-Ca cells.…”

Section: Introductionmentioning

confidence: 63%

“…LTLT-Ca were generated from MCF7-Ca as previously described [2] and were maintained in phenol red-free modified IMEM supplemented with 5 % CDT-FBS, 1 % P/S, 750 lg/mL G418 and 1 lM letrozole. Ac-1 cells (MCF-7 cells stably transfected with aromatase gene in our laboratory) were used to develop the Ac1ANAR cell line as described previously [6]. Ac1ANAR were maintained in IMEM containing 5 % CDT-FBS, 1 % P/S, 800 lg/mL G418 and 2 lM anastrozole.…”

Section: Methodsmentioning

confidence: 99%

“…We have used letrozoleresistant LTLT-Ca and anastrozole-resistant Ac1ANAR for our studies. Both cell lines demonstrate a downregulation of ERa and upregulation of HER2 protein expression [2,6], as well as increased TIC characteristics [5,7] when compared to their AI-sensitive parental cell lines. LTLT-Ca and Ac1ANAR were treated with ATRA, ENT, or the combination for 96 h and expression of HER2 was assessed via western blot.…”

Section: Combination Ent and Atra Inhibited Her2 Expression And Cell mentioning

confidence: 99%

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Histone deacetylase inhibitor entinostat in combination with a retinoid downregulates HER2 and reduces the tumor initiating cell population in aromatase inhibitor-resistant breast cancer

Schech

Shah

et al. 2015

Breast Cancer Res Treat

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Resistance to aromatase inhibitors (AIs) involves increased HER2. One mechanism by which HER2 may mediate resistance is through expansion of the tumor initiating cell (TIC) population. This study investigates whether combining all-trans retinoic acid (ATRA) and histone deacetylase inhibitor entinostat (ENT) can inhibit TICs and HER2 in AI-resistant cells and tumors. Modulation of cell viability and HER2 expression were assessed in AI-resistant cells treated with ATRA + ENT. Letrozole-resistant LTLT-Ca cells treated with ATRA + ENT were assayed for changes in TIC characteristics, such as TIC markers (BCRP, ALDH, and BMI-1), side population (SP), and mammosphere formation. Xenograft tumors of MCF-7Ca cells made resistant to letrozole were treated with ATRA, ATRA + letrozole, ATRA + ENT, or ATRA + ENT + letrozole. Resulting tumors were assayed for changes in TIC characteristics. Patient samples taken pre- and post-AI treatment were analyzed for changes in ERα and HER2 protein expression. Treatment with ATRA + ENT reduced HER2 expression and viability (P < 0.001) in AI-resistant cells, as well as decreased SP (P < 0.0001), mammosphere formation (P < 0.01), and expression of TIC molecular markers (P < 0.01) in LTLT-Ca. A reduction in tumor growth rate was observed in mice treated with ENT + ATRA + letrozole when compared to mice treated with single agents (P < 0.0001) or ENT + ATRA (P = 0.02). Decreased TIC characteristics, including mammosphere formation (P < 0.05), were observed in tumors from the triple combination. An increase in HER2 and downregulation in ERα protein expression was observed in patients upon resistance to AI (P < 0.005). These studies indicate that the combination of ATRA and ENT inhibits the TIC population of AI-resistant cells and may be effective in reducing tumor recurrence.

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Effect of selumetinib on the growth of anastrozole-resistant tumors

Cited by 12 publications

References 41 publications

Treatment with aromatase inhibitors stimulates the expression of epidermal growth factor receptor-1 and neuregulin 1 in ER positive/HER-2/neu non-amplified primary breast cancers

Treatment with aromatase inhibitors stimulates the expression of epidermal growth factor receptor-1 and neuregulin 1 in ER positive/HER-2/neu non-amplified primary breast cancers

Stimulus-dependent differences in signalling regulate epithelial-mesenchymal plasticity and change the effects of drugs in breast cancer cell lines

Histone deacetylase inhibitor entinostat in combination with a retinoid downregulates HER2 and reduces the tumor initiating cell population in aromatase inhibitor-resistant breast cancer

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