Strong antitumor synergy between DNA crosslinking and HSP90 inhibition causes massive premitotic DNA fragmentation in ovarian cancer cells

Krämer, Daniela; Stark, Nadine; Schulz-Heddergott, Ramona; Erytch, Norman; Edmunds, Shelley J.; Roßmann, Laura; Bastians, Holger; Concin, Nicole; Moll, Ute M.; Dobbelstein, Matthias

doi:10.1038/cdd.2016.124

Cited by 16 publications

(18 citation statements)

References 59 publications

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“…Onalespib for example, has been found to sensitize malignant glioma cells to temozolomide. The HSP90 antagonist ganetespib, has recently been investigated for sensitizing effects in ovarian cancer and pancreatic cancer cells to chemotherapy 25 and radiochemotherapy 26 , respectively. The HSP90 antagonist NVP-AUY922 potentiated anti-cancer effects of a BCL-2 inhibitor in small cell lung cancer 27 and demonstrated synergy in combination with trastuzumab in breast cancer 28 .…”

Section: Discussionmentioning

confidence: 99%

The HSP90 inhibitor Onalespib exerts synergistic anti-cancer effects when combined with radiotherapy: an in vitro and in vivo approach

Spiegelberg

Abramenkovs

Mortensen

et al. 2020

Sci Rep

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Oncogenic client-proteins of the chaperone Heat shock protein 90 (HSP90) insure unlimited tumor growth and are involved in resistance to chemo-and radiotherapy. The HSP90 inhibitor Onalespib initiates the degradation of oncoproteins, and might also act as a radiosensitizer. The aim of this study was therefore to evaluate the efficacy of Onalespib in combination with external beam radiotherapy in an in vitro and in vivo approach. Onalespib downregulated client proteins, lead to increased apoptosis and caused DNA-double-strands. Monotherapy and combination with radiotherapy reduced colony formation, proliferation and migration assessed in radiosensitive HCT116 and radioresistant A431 cells. In vivo, a minimal treatment regimen for 3 consecutive days of Onalespib (3 × 10 mg/kg) doubled survival, whereas Onalespib with radiotherapy (3 × 2 Gy) caused a substantial delay in tumor growth and prolonged the survival by a factor of 3 compared to the HCT116 xenografted control group. Our results demonstrate that Onalespib exerts synergistic anti-cancer effects when combined with radiotherapy, most prominent in the radiosensitive cell models. We speculate that the depletion and downregulation of client proteins involved in signalling, migration and DNA repair mechanisms is the cause. Thus, individually, or in combination with radiotherapy Onalespib inhibits tumor growth and has the potential to improve radiotherapy outcomes, prolonging the overall survival of cancer patients.

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Section: Discussionmentioning

confidence: 99%

The HSP90 inhibitor Onalespib exerts synergistic anti-cancer effects when combined with radiotherapy: an in vitro and in vivo approach

Spiegelberg

Abramenkovs

Mortensen

et al. 2020

Sci Rep

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“…In nearly all experiments, we observed that Ganetespib considerably potentiates cell killing by hyperthermia, in line with a recent study that reported enhancement of the effects of hyperthermia by 17-DMAG [ 47 , 48 ]. It is worth noting that prolonged administration of Ganetespib alone can also sensitize cancer cells to radiation and some chemotherapeutic drugs [ 49 – 51 ]. Second, the increased inhibition of HR (and, potentially, other DNA repair mechanisms) by hyperthermia and Ganetespib sensitizes cells to multiple DSB-inducing agents, indirectly increasing their cytotoxicity.…”

Section: Discussionmentioning

confidence: 99%

Boosting the effects of hyperthermia-based anticancer treatments by HSP90 inhibition

Vriend¹,

Tempel

Oei³

et al. 2017

Oncotarget

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Hyperthermia – application of supra-physiological temperatures to cells, tissues or organs – is a pleiotropic treatment that affects most aspects of cellular metabolism, but its effects on DNA are of special interest in the context of cancer research and treatment. Hyperthermia inhibits repair of various DNA lesions, including double-strand breaks (DSBs), making it a powerful radio- and chemosensitizer, with proven clinical efficacy in therapy of various types of cancer, including tumors of head and neck, bladder, breast and cervix. Among the challenges for hyperthermia-based therapies are the transient character of its effects, the technical difficulties in maintaining uniformly elevated tumor temperature and the acquisition of thermotolerance. Approaches to reduce or eliminate these challenges could simplify the application of hyperthermia, boost its efficacy and improve treatment outcomes. Here we show that a single, short treatment with a relatively low dose of HSP90 inhibitor Ganetespib potentiates cytotoxic as well as radio- and chemosensitizing effects of hyperthermia and reduces thermotolerance in cervix cancer cell lines. Ganetespib alone, applied at this low dose, has virtually no effect on survival of non-heated cells. Our results thus suggest that HSP90 inhibition can be a safe, simple and efficient approach to improving hyperthermia treatment efficacy and reducing thermotolerance, paving the way for in vivo studies.

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“…In the research of Kramer et al, it was shown that by jointly inhibiting DNA repair and cell cycle control mechanisms, HSP90 inhibitor ganetespib blocked the degradation of FANCA and the imbalance of nuclease DNA2. On this basis, ganetespib enhanced the anti‐tumour efficacy of carboplatin, thereby triggering overall chromosomal destruction, abnormal mitosis and cell death in ovarian cancer cells 46 . It has been reported that heterozygous carriers of FA gene mutations will not cause FA phenotype, but may increase the risk of cancer.…”

Section: Discussionmentioning

confidence: 99%

The identification of six risk genes for ovarian cancer platinum response based on global network algorithm and verification analysis

Xing

Zhang

et al. 2020

J Cellular Molecular Medi

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Ovarian cancer is the most lethal gynaecological cancer, and resistance of platinum‐based chemotherapy is the main reason for treatment failure. The aim of the present study was to identify candidate genes involved in ovarian cancer platinum response by analysing genes from homologous recombination and Fanconi anaemia pathways. Associations between these two functional genes were explored in the study, and we performed a random walk algorithm based on reconstructed gene‐gene network, including protein‐protein interaction and co‐expression relations. Following the random walk, all genes were ranked and GSEA analysis showed that the biological functions focused primarily on autophagy, histone modification and gluconeogenesis. Based on three types of seed nodes, the top two genes were utilized as examples. We selected a total of six candidate genes (FANCA, FANCG, POLD1, KDM1A, BLM and BRCA1) for subsequent verification. The validation results of the six candidate genes have significance in three independent ovarian cancer data sets with platinum‐resistant and platinum‐sensitive information. To explore the correlation between biomarkers and clinical prognostic factors, we performed differential analysis and multivariate clinical subgroup analysis for six candidate genes at both mRNA and protein levels. And each of the six candidate genes and their neighbouring genes with a mutation rate greater than 10% were also analysed by network construction and functional enrichment analysis. In the meanwhile, the survival analysis for platinum‐treated patients was performed in the current study. Finally, the RT‐qPCR assay was used to determine the performance of candidate genes in ovarian cancer platinum response. Taken together, this research demonstrated that comprehensive bioinformatics methods could help to understand the molecular mechanism of platinum response and provide new strategies for overcoming platinum resistance in ovarian cancer treatment.

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Strong antitumor synergy between DNA crosslinking and HSP90 inhibition causes massive premitotic DNA fragmentation in ovarian cancer cells

Cited by 16 publications

References 59 publications

The HSP90 inhibitor Onalespib exerts synergistic anti-cancer effects when combined with radiotherapy: an in vitro and in vivo approach

The HSP90 inhibitor Onalespib exerts synergistic anti-cancer effects when combined with radiotherapy: an in vitro and in vivo approach

Boosting the effects of hyperthermia-based anticancer treatments by HSP90 inhibition

The identification of six risk genes for ovarian cancer platinum response based on global network algorithm and verification analysis

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