The proteasome inhibitor Bortezomib (Velcade) as potential inhibitor of estrogen receptor-positive breast cancer

Thaler, Sonja; Thiede, Gitta; Hengstler, Jan G.; Schad, Arno; Schmidt, Marcus; Sleeman, Jonathan

doi:10.1002/ijc.29404

Cited by 32 publications

(33 citation statements)

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“…Our results also support the hypothesis that resveratrol may exert its anti-ERα action by impairing proteasome-mediated ERα activation. Interestingly, UPS has been described as necessary for a correct activation of ERα [40] and some proteasome inhibitors have been shown to repress ERα gene expression [41, 42]. Moreover, a recently published work has proposed that mTORC1 inhibition activates the Ubiquitin/Proteasome System (UPS) and autophagy [43], thus sustaining an inverse correlation between mTOR signaling and proteasome activity.…”

Section: Resultsmentioning

confidence: 99%

“…For the in vitro experiments resveratrol was dissolved in DMSO (Sigma) and then diluted in complete DMEM to usage concentrations (10-100 μM). 17β-estradiol (Calbiochem) was used as control estrogen treatment (stock solution 40 mM in 100% ethanol and diluted in complete DMEM to 10 nM), as previously described [41]. Cells were treated for 24 hours with resveratrol/17β-estradiol- or vehicle-containing medium (0.02% DMSO).…”

Section: Resultsmentioning

confidence: 99%

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Resveratrol fuels HER2 and ERα-positive breast cancer behaving as proteasome inhibitor

Andreani

Bartolacci

Wijnant

et al. 2017

Aging

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The phytoestrogen resveratrol has been reported to possess cancer chemo-preventive activity on the basis of its effects on tumor cell lines and xenograft or carcinogen-inducible in vivo models. Here we investigated the effects of resveratrol on spontaneous mammary carcinogenesis using Δ16HER2 mice as HER2+/ERα+ breast cancer model. Instead of inhibiting tumor growth, resveratrol treatment (0.0001% in drinking water; daily intake of 4μg/mouse) shortened tumor latency and enhanced tumor multiplicity in Δ16HER2 mice. This in vivo tumor-promoting effect of resveratrol was associated with up-regulation of Δ16HER2 and down-regulation of ERα protein levels and was recapitulated in vitro by murine (CAM6) and human (BT474) tumor cell lines. Our results demonstrate that resveratrol, acting as a proteasome inhibitor, leads to Δ16HER2 accumulation which favors the formation of Δ16HER2/HER3 heterodimers. The consequential activation of downstream mTORC1/p70S6K/4EBP1 pathway triggers cancer growth and proliferation. This study provides evidence that resveratrol mechanism of action (and hence its effects) depends on the intrinsic molecular properties of the cancer model under investigation, exerting a tumor-promoting effect in luminal B breast cancer subtype models.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Resveratrol fuels HER2 and ERα-positive breast cancer behaving as proteasome inhibitor

Andreani

Bartolacci

Wijnant

et al. 2017

Aging

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“…Remarkably, the fact that E2 is still able to trigger ERα degradation in the presence of carfilzomib suggests that this drug does not bind to ERα and that its effects depend on the ability of the drug to inhibit the 26S proteasome. Accordingly, treatment of BC cell lines with other inhibitors of 26S proteasome activity (e.g., bortezomib -Velcade®) reduces ERα levels and consequently prevents receptor-dependent signaling [39]. The apparent paradox that 26S proteasome inhibitors reduce the levels of ERα, which turnover is, at least in part, controlled by the 26S proteasome itself can be reconciled by considering that the irreversible inhibition of 26S proteasome leads to a high accumulation of ubiquitinated species, which cells remove by activating autophagy [40,41].…”

Section: Discussionmentioning

confidence: 99%

A functional drug re-purposing screening identifies carfilzomib as a drug preventing 17β-estradiol: ERα signaling and cell proliferation in breast cancer cells

Busonero

Leone

Klemm

et al. 2017

Preprint

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“…to Bortezomib (proteasome activity inhibitor 35,36 ), with a significant synergic action at several dosages, suggesting a novel therapeutic strategy to be further explored in preclinical models of cluster 2 tumours. These observations indicate that our study succeeded in: 1) clustering tumours highlighting common functional mechanisms related to their transcriptional profile, and 2) selecting genes with a relevant functional role in the studied tumours, thus amenable of drug targeting.…”

Section: Discussionmentioning

confidence: 99%

Network integration of multi-tumour omics data suggests novel targeting strategies

Valle

Menichetti

Simonetti

et al. 2017

Preprint

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We characterize different tumour types in the search for multi-tumour drug targets, in particular aiming for drug repurposing or novel drug combinations. Starting from 11 tumour types from The Cancer Genome Atlas, we obtain three clusters based on transcriptomic correlation profiles. A network-based analysis, integrating gene expression profiles and protein interactions of cancer-related genes, allowed us to define three cluster-specific signatures, with genes belonging to NF-κB signaling, chromosomal instability, ubiquitin-proteasome system, DNA metabolism, and apoptosis biological processes. These signatures have been characterized by different approaches based on mutational, pharmacological and clinical evidences, demonstrating the validity of our selection. Moreover, we defined new pharmacological strategies validated by in vitro experiments that showed inhibition of cell growth in two tumour cell lines, with significant synergistic effect. Our study thus provides a list of genes and pathways with the potential to be used, singularly or in combination, for the design of novel treatment strategies.

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The proteasome inhibitor Bortezomib (Velcade) as potential inhibitor of estrogen receptor-positive breast cancer

Cited by 32 publications

References 50 publications

Resveratrol fuels HER2 and ERα-positive breast cancer behaving as proteasome inhibitor

Resveratrol fuels HER2 and ERα-positive breast cancer behaving as proteasome inhibitor

A functional drug re-purposing screening identifies carfilzomib as a drug preventing 17β-estradiol: ERα signaling and cell proliferation in breast cancer cells

Network integration of multi-tumour omics data suggests novel targeting strategies

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