Your search keyword '"Sarah Jurmeister"' showing total 9 results

1. Identification of potential therapeutic targets in prostate cancer through a cross‐species approach

Author

Sarah Jurmeister, Antonio Ramos‐Montoya, Chiranjeevi Sandi, Nelma Pértega‐Gomes, Karan Wadhwa, Alastair D Lamb, Mark J Dunning, Jan Attig, Jason S Carroll, Lee GD Fryer, Sérgio L Felisbino, and David E Neal

Subjects

cross‐species analysis, MELK, mouse models, new cancer targets, prostate cancer, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Genetically engineered mouse models of cancer can be used to filter genome‐wide expression datasets generated from human tumours and to identify gene expression alterations that are functionally important to cancer development and progression. In this study, we have generated RNAseq data from tumours arising in two established mouse models of prostate cancer, PB‐Cre/PtenloxP/loxP and p53loxP/loxPRbloxP/loxP, and integrated this with published human prostate cancer expression data to pinpoint cancer‐associated gene expression changes that are conserved between the two species. To identify potential therapeutic targets, we then filtered this information for genes that are either known or predicted to be druggable. Using this approach, we revealed a functional role for the kinase MELK as a driver and potential therapeutic target in prostate cancer. We found that MELK expression was required for cell survival, affected the expression of genes associated with prostate cancer progression and was associated with biochemical recurrence.

Published

2018

2. HES6 drives a critical AR transcriptional programme to induce castration‐resistant prostate cancer through activation of an E2F1‐mediated cell cycle network

Author

Antonio Ramos‐Montoya, Alastair D Lamb, Roslin Russell, Thomas Carroll, Sarah Jurmeister, Nuria Galeano‐Dalmau, Charlie E Massie, Joan Boren, Helene Bon, Vasiliki Theodorou, Maria Vias, Greg L Shaw, Naomi L Sharma, Helen Ross‐Adams, Helen E Scott, Sarah L Vowler, William J Howat, Anne Y Warren, Richard F Wooster, Ian G Mills, and David E Neal

Subjects

androgen receptor, castrate‐resistant prostate cancer, gene expression signature, HES6, PLK1, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Castrate‐resistant prostate cancer (CRPC) is poorly characterized and heterogeneous and while the androgen receptor (AR) is of singular importance, other factors such as c‐Myc and the E2F family also play a role in later stage disease. HES6 is a transcription co‐factor associated with stem cell characteristics in neural tissue. Here we show that HES6 is up‐regulated in aggressive human prostate cancer and drives castration‐resistant tumour growth in the absence of ligand binding by enhancing the transcriptional activity of the AR, which is preferentially directed to a regulatory network enriched for transcription factors such as E2F1. In the clinical setting, we have uncovered a HES6‐associated signature that predicts poor outcome in prostate cancer, which can be pharmacologically targeted by inhibition of PLK1 with restoration of sensitivity to castration. We have therefore shown for the first time the critical role of HES6 in the development of CRPC and identified its potential in patient‐specific therapeutic strategies.

Published

2014

3. HES6 drives a critical AR transcriptional programme to induce castration‐resistant prostate cancer through activation of an E2F1‐mediated cell cycle network

Author

Charles E. Massie, Antonio Ramos-Montoya, Sarah L. Vowler, N L Sharma, Helene Bon, David E. Neal, Vasiliki Theodorou, Helen Ross-Adams, Richard F. Wooster, H Scott, Sarah Jurmeister, Greg Shaw, Joan Boren, Anne Y. Warren, Nuria Galeano-Dalmau, Maria Vias, Alastair D. Lamb, Roslin Russell, Ian G. Mills, William J. Howat, and Thomas L. Carroll

Subjects

Male, Molecular Sequence Data, Cell Cycle Proteins, Biology, gene expression signature, Prostate cancer, Mice, SDG 3 - Good Health and Well-being, androgen receptor, castrate-resistant prostate cancer, medicine, Basic Helix-Loop-Helix Transcription Factors, E2F1, Animals, Humans, Transcription factor, Research Articles, Regulation of gene expression, Gene Expression Profiling, Prostatic Neoplasms, E2F1 Transcription Factor, Sequence Analysis, DNA, Cell cycle, medicine.disease, 3. Good health, Androgen receptor, Repressor Proteins, Disease Models, Animal, Gene Expression Regulation, Receptors, Androgen, Cancer research, Molecular Medicine, HES6, Stem cell, PLK1

Abstract

Castrate‐resistant prostate cancer (CRPC) is poorly characterized and heterogeneous and while the androgen receptor (AR) is of singular importance, other factors such as c‐Myc and the E2F family also play a role in later stage disease. HES6 is a transcription co‐factor associated with stem cell characteristics in neural tissue. Here we show that HES6 is up‐regulated in aggressive human prostate cancer and drives castration‐resistant tumour growth in the absence of ligand binding by enhancing the transcriptional activity of the AR, which is preferentially directed to a regulatory network enriched for transcription factors such as E2F1. In the clinical setting, we have uncovered a HES6‐associated signature that predicts poor outcome in prostate cancer, which can be pharmacologically targeted by inhibition of PLK1 with restoration of sensitivity to castration. We have therefore shown for the first time the critical role of HES6 in the development of CRPC and identified its potential in patient‐specific therapeutic strategies.

Published

2019

4. Transcriptomic analysis reveals inhibition of androgen receptor activity by AMPK in prostate cancer cells

Author

Antonio Ramos-Montoya, David E. Neal, Lee G. D. Fryer, and Sarah Jurmeister

Subjects

AMPK, Male, medicine.medical_specialty, cancer metabolism, AMP-Activated Protein Kinases, Transfection, Prostate cancer, AMP-activated protein kinase, Internal medicine, medicine, Tumor Cells, Cultured, Humans, RNA, Small Interfering, Transcription factor, Regulation of gene expression, Cell Nucleus, biology, Kinase, Gene Expression Profiling, medicine.disease, prostate cancer, Androgen receptor, Gene Expression Regulation, Neoplastic, Prostatic Neoplasms, Castration-Resistant, Endocrinology, Oncology, Receptors, Androgen, Cancer research, biology.protein, Signal transduction, transcription, Research Paper, Signal Transduction

Abstract

// Sarah Jurmeister 1 , Antonio Ramos-Montoya 1 , David E. Neal 1,2 and Lee G.D. Fryer 1 1 Uro-Oncology Research Group, Cancer Research UK Cambridge Institute, University of Cambridge, Li Ka Shing Centre, Robinson Way, UK 2 Dept of Urology, University of Cambridge, S4, Dept of Oncology, Addenbrooke’s Hospital, UK Correspondence: Lee Fryer, email: // Keywords : Androgen receptor, AMPK, prostate cancer, cancer metabolism, transcription Received : March 24, 2014 Accepted : May 19, 2014 Published : May 21, 2014 Abstract Metabolic alterations contribute to prostate cancer development and progression; however, the role of the central metabolic regulator AMP-activated protein kinase (AMPK) remains controversial. The androgen receptor (AR), a key driver of prostate cancer, regulates prostate cancer cell metabolism by driving the expression of a network of metabolic genes and activates AMPK through increasing the expression of one of its upstream kinases. To more clearly define the role of AMPK in prostate cancer, we performed expression profiling following pharmacologic activation of this kinase. We found that genes down-regulated upon AMPK activation were over-expressed in prostate cancer, consistent with a tumour suppressive function of AMPK. Strikingly, we identified the AR as one of the most significantly enriched transcription factors mediating gene expression changes downstream of AMPK signalling in prostate cancer cells. Activation of AMPK inhibited AR transcriptional activity and reduced androgen-dependent expression of known AR target genes. Conversely, knock-down of AMPK increased AR activity. Modulation of AR expression could not explain these effects. Instead, we observed that activation of AMPK reduced nuclear localisation of the AR. We thus propose the presence of a negative feedback loop in prostate cancer cells whereby AR activates AMPK and AMPK feeds back to limit AR-driven transcription.

Published

2014

5. Downregulation of androgen receptor transcription by promoter g-quadruplex stabilization as a potential alternative treatment for castrate-resistant prostate cancer

Author

Lee G. D. Fryer, Stephan A. Ohnmacht, Sarah Jurmeister, David E. Neal, Marco Di Antonio, Antonio Ramos-Montoya, Thomas J. Mitchell, Pierre Murat, Marialuisa Micco, Shankar Balasubramanian, and Stephen Neidle

Subjects

Male, Transcriptional Activation, Down-Regulation, Antineoplastic Agents, Biology, Naphthalenes, Imides, Biochemistry, Prostate cancer, Downregulation and upregulation, Transcription (biology), Cell Line, Tumor, medicine, Fluorescence Resonance Energy Transfer, Humans, heterocyclic compounds, Promoter Regions, Genetic, Gene, Nuclear Magnetic Resonance, Biomolecular, Cell Proliferation, Regulation of gene expression, Reporter gene, Circular Dichroism, Prostate, Prostatic Neoplasms, Promoter, medicine.disease, Molecular biology, Androgen receptor, G-Quadruplexes, Gene Expression Regulation, Neoplastic, Receptors, Androgen, Spectrophotometry, Ultraviolet

Abstract

Androgen receptor (AR) signaling remains an important regulatory pathway in castrate-resistant prostate cancer, and its transcriptional downregulation could provide a new line of therapy. A number of small-molecule ligands have previously demonstrated the ability to stabilize G-quadruplex structures and affect gene transcription for those genes whose promoters contain a quadruplex-forming sequence. Herein, we report the probable formation of new G-quadruplex structure present in the AR promoter in a transcriptionally important location. NMR spectroscopy, circular dichroism, UV spectroscopy, and UV thermal melting experiments for this sequence are consistent with G-quadruplex formation. Fluorescence resonance energy transfer (FRET) melting studies have identified a novel compound, MM45, which appears to stabilize this G-quadruplex at submicromolar concentrations. The effects of MM45 have been investigated in prostate cancer cell lines where it has been shown to inhibit cell growth. A reporter assay intended to isolate the effect of MM45 on the G-quadruplex sequence showed dose-dependent transcriptional repression only when the AR promoter G-quadruplex sequence is present. Dose-dependent transcriptional repression of the AR by MM45 has been demonstrated at both a protein and mRNA level. This proof of concept study paves the route toward a potential alternative treatment pathway in castrate-resistant prostate cancer.

Published

2013

6. Abstract 389: The dual mTOR inhibitor, AZD2014, and castration increase intra-tumoral immune cell infiltration and anti-tumour activity in a genetically engineered mouse model of prostate cancer

Author

Frances M. Richards, Sarah Jurmeister, Robert W. Wilkinson, Antonio Ramos-Montoya, Duncan I. Jodrell, Karan Wadhwa, Suzanne Mosely, Chiranjeevi Sandi, Sabina Cosulich, Barry R. Davies, Sergio L. Filisbino, Michelle Morrow, A. Hughes, and Simon Pacey

Subjects

Cancer Research, Chemotherapy, medicine.medical_specialty, biology, business.industry, medicine.medical_treatment, Cancer, medicine.disease, mTORC2, chemistry.chemical_compound, Prostate cancer, Castration, Endocrinology, Oncology, chemistry, Internal medicine, biology.protein, Cancer research, Medicine, PTEN, business, Protein kinase B, PI3K/AKT/mTOR pathway

Abstract

Background: Medical therapy for men with prostate cancer (PCa) is evolving, including recent evidence to support the use of chemotherapy for men with hormone sensitive disease. PI3K/AKT/mTOR pathway aberrations are common in patients with primary PCa and almost universal in metastatic tumours. The mTOR pathway acts as a central regulator of tumour cell metabolism, proliferation, cell cycle progression and immune regulation. The aim of this study was to investigate the effects of mTOR inhibitor AZD2014 on tumour growth and immune infiltration in a genetically engineered mouse model of PCa. Methods: PtenL/L;PB-Cre4 mice, which developed invasive hormone-sensitive prostate tumours between 10-14 months of age, were enrolled (n = 13-15 per group) and treated with AZD2014 (15mg/Kg) or vehicle orally for 14 doses (QD 5/7) with or without castration. Tumour volumes were assessed by ultrasound imaging. Tumour samples were collected within 4 hours post 14th dose for histological and molecular analysis. Results: AZD2014 was well tolerated, no overt toxicity was observed. Mean plasma concentrations of AZD2014 were 4.4±2.1μM at time of tumour sampling. AZD2014 alone or AZD2014+castration inhibited mTORC1 and mTORC2 activity as demonstrated by reduced p4EBP1(Thr37/46) 48%±27% (P Conclusion: These data confirm the anti cancer effect of AZD2014 in this PCa model. Furthermore, AZD2014+castration was more effective than either treatment as a single agent. The increased intra-tumoral T cell infiltration observed may have contributed to the anti-tumour effect. Further studies are ongoing to maximise this therapeutic effect and will inform current clinical studies in men with hormone sensitive, high risk prostate cancer. Citation Format: Chiranjeevi Sandi, Antonio Ramos-Montoya, Sergio L. Filisbino, Adina Hughes, Suzanne Mosely, Michelle Morrow, Robert W. Wilkinson, Sarah Jurmeister, Karan Wadhwa, Frances M. Richards, Duncan I. Jodrell, Sabina Cosulich, Barry R. Davies, Simon Pacey. The dual mTOR inhibitor, AZD2014, and castration increase intra-tumoral immune cell infiltration and anti-tumour activity in a genetically engineered mouse model of prostate cancer. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 389.

Published

2016

7. MicroRNA-200c represses migration and invasion of breast cancer cells by targeting actin-regulatory proteins FHOD1 and PPM1F

Author

Ozgur Sahin, Marek Baumann, Jitao David Zhang, Ioanna Keklikoglou, Sarah Jurmeister, Aoife Ward, Stefan Wiemann, Stefan Uhlmann, and Aleksandra Balwierz

Subjects

Fetal Proteins, Serum Response Factor, Stress fiber, Myosin Light Chains, Oncogene Proteins, Fusion, Down-Regulation, Formins, Breast Neoplasms, Biology, Cell Movement, Transforming Growth Factor beta, Cell Line, Tumor, Stress Fibers, Serum response factor, Coactivator, Phosphoprotein Phosphatases, Humans, Neoplasm Invasiveness, Cytoskeleton, Molecular Biology, Transcription factor, Actin, Nuclear Proteins, Cell migration, Cell Biology, Articles, Actin cytoskeleton, Cell biology, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, MicroRNAs, Trans-Activators, Female, Cardiac Myosins

Abstract

MicroRNA-200c (miR-200c) has been shown to suppress epithelial-mesenchymal transition (EMT), which is attributed mainly to targeting of ZEB1/ZEB2, repressors of the cell-cell contact protein E-cadherin. Here we demonstrated that modulation of miR-200c in breast cancer cells regulates cell migration, cell elongation, and transforming growth factor β (TGF-β)-induced stress fiber formation by impacting the reorganization of cytoskeleton that is independent of the ZEB/E-cadherin axis. We identified FHOD1 and PPM1F, direct regulators of the actin cytoskeleton, as novel targets of miR-200c. Remarkably, expression levels of FHOD1 and PPM1F were inversely correlated with the level of miR-200c in breast cancer cell lines, breast cancer patient samples, and 58 cancer cell lines of various origins. Furthermore, individual knockdown/overexpression of these target genes phenocopied the effects of miR-200c overexpression/inhibition on cell elongation, stress fiber formation, migration, and invasion. Mechanistically, targeting of FHOD1 by miR-200c resulted in decreased expression and transcriptional activity of serum response factor (SRF), mediated by interference with the translocation of the SRF coactivator mycocardin-related transcription factor A (MRTF-A). This finally led to downregulation of the expression and phosphorylation of the SRF target myosin light chain 2 (MLC2) gene, required for stress fiber formation and contractility. Thus, miR-200c impacts on metastasis by regulating several EMT-related processes, including a novel mechanism involving the direct targeting of actin-regulatory proteins.

Published

2011

8. Abstract A123: Preclinical evaluation of dual mTOR inhibitor, AZD2014, in prostate cancer

Author

Basetti Madhu, Karan Wadhwa, Frances M. Richards, David E. Neal, Sabina Cosulich, Chiranjeevi Sandi, Antonio Ramos-Montoya, Barry R. Davies, Sérgio Luis Felisbino, Duncan I. Jodrell, John R. Griffiths, Sarah Jurmeister, Simon Pacey, Richards, Fran [0000-0001-7947-7853], Jodrell, Duncan [0000-0001-9360-1670], Pacey, Simon [0000-0002-3303-7577], and Apollo - University of Cambridge Repository

Subjects

Urologic Diseases, Oncology, Aging, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, 32 Biomedical and Clinical Sciences, mTORC2, Prostate cancer, Prostate, Internal medicine, Medicine, PTEN, 3202 Clinical Sciences, PI3K/AKT/mTOR pathway, Cancer, biology, business.industry, Prostatectomy, Prostate Cancer, 3211 Oncology and Carcinogenesis, medicine.disease, medicine.anatomical_structure, Immunology, biology.protein, Biomarker (medicine), business

Abstract

Background: An estimated 220,800 cases and 27,540 deaths from prostate cancer (PCa) will occur in the USA during 2015. Altered PI3K/AKT/mTOR signalling contributes to prostate cancer progression and transition to androgen-independent disease, for example one study reported 42% of primary and 100% of metastatic PCa tumours exhibited mutations, altered expression or copy number variations within this pathway. First generation mTOR inhibitors (preferentially inhibit mTORC1), have had limited anti-cancer effect in patients with PCa, possibly due to negative feedback activation of the AKT pathway via mTORC2. The dual mTORC1/2 inhibitor, AZD2014, may overcome this liability. Using a genetically engineered PTEN conditional mouse model (Ptenloxp/loxp;PB-Cre4), we have investigated the effects of AZD2014. The studies complement a clinical trial (NCT02064608) of AZD2014, given to men before radical prostatectomy and are timed for when invasive prostate carcinomas develop in the model around 10-14 months prior to onset of resistance to castration through AKT pathway activation. AZD2014, 15mg/kg daily, oral (with or without castration) or vehicle were administered for 14 days. Results: AZD2014 was well tolerated with no overt toxicity observed. Pharmacokinetic (PK) analysis revealed mean concentrations of 4.4±2.1μM of AZD2014 in the plasma samples collected 4 hours after day 14 dose. AZD2014 alone or combined with castration inhibited mTORC1 and mTORC2 measured by reductions in p4EBP1(Thr37/46) by approximately 48%±27% (p Conclusions: Short term (14 days) treatment with AZD2014 with or without castration was associated with both pharmacodynamic and anti-tumour effects. The t-Cho/Cr ratio, previously reported as positively correlated with Gleason score in PCa patients, might be, in addition to our standard mTOR PD markers, utilised as a non-invasive biomarker of AZD2014 activity. The primary and phenotypic biomarker effects of monotherapy with AZD2014 in this relevant genetically engineered mouse model of prostate cancer will be compared with paired biopsies from the ongoing exploratory window study in the prostate cancer patients prior to prostatectomy, and may inform potential novel combination approaches that are translatable to the clinic. Citation Format: Chiranjeevi Sandi, Antonio Ramos-Montoya, Sergio L. Felisbino, Sarah Jurmeister, Basetti Madhu, Karan Wadhwa, John R. Griffiths, Frances M. Richards, Duncan I. Jodrell, David E. Neal, Sabina Cosulich, Barry Davies, Simon Pacey. Preclinical evaluation of dual mTOR inhibitor, AZD2014, in prostate cancer. [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2015 Nov 5-9; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2015;14(12 Suppl 2):Abstract nr A123.

Published

2015

9. A lactate shuttle system between tumour and stromal cells is associated with poor prognosis in prostate cancer

Author

José Ramón Vizcaíno, Carlos Lopes, Nelma Pértega-Gomes, Sarah Jurmeister, Fátima Baltazar, Jan Attig, and Universidade do Minho

Subjects

Biochemical recurrence, Male, Monocarboxylic Acid Transporters, Poor prognosis, Pathology, medicine.medical_specialty, Cancer Research, Stromal cell, Muscle Proteins, Biology, Malignant transformation, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, medicine, Genetics, Humans, Reverse Warburg effect, Lactic Acid, Monocarboxylate transporters, 030304 developmental biology, Neoplasm Staging, Prostatectomy, 0303 health sciences, Science & Technology, Symporters, Cancer, Prostatic Neoplasms, Biological Transport, Fibroblasts, Middle Aged, Prostate-Specific Antigen, medicine.disease, Cancer associated fibroblasts, 3. Good health, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Hormonal therapy, Kallikreins, Stromal Cells, Energy Metabolism, Research Article

Abstract

Background In a malignant tumour, cancer cells are embedded in stromal cells, namely cancer-associated fibroblasts (CAFs). These CAFs are now accepted as important players in cancer dynamics, being involved in tumour growth and progression. Although there are various reports on the interaction between tumour and stromal cells, the clinico-pathological significance of this cross-talk is still largely unknown. In this study, we aimed to characterise the expression of key metabolic proteins involved in glucose transport, pyruvate/lactate shuttle system, glycolytic metabolism and fatty acid oxidation in CAFs and tumour cells in different stages of malignant transformation. We further aimed to contextualise the clinico-pathological significance of these protein expression profiles with reference to known prognostic indicators, including biochemical recurrence in pT stage. Methods Prostate tissues were obtained from 480 patients with a median age of 64 years following radical prostatectomy with no previous hormonal therapy. Tissues were analysed for the expression of several key metabolism-related proteins in glands and surrounding fibroblasts by immunohistochemistry. Reliable markers of prognosis such as pT stage and biochemical recurrence were assessed for each case. Results We observed that prostate cancer cells did not rely mainly on glycolytic metabolism, while there was a high expression of MCT4 and CAIX - in CAFs. This corroborates the hypothesis of the "Reverse Warburg effect" in prostate cancer, in which fibroblasts are under oxidative stress and express CAIX, an established hypoxia marker. We found that alterations in the expression of metabolism-related proteins were already evident in the early stages of malignant transformation, suggesting the continuing alteration of CAFs from an early stage. Additionally, and for the first time, we show that cases showing high MCT4 expression in CAFs with concomitant strong MCT1 expression in prostate cancer (PCa) cells are associated with poor clinical outcome, namely pT3 stage of the tumour. Conclusions In summary, this work demonstrates for the first time the clinico-pathological significance of the lactate shuttle in prostate cancer. It also suggests that other alterations in CAFs may be useful prognostic factors, and further supports the use of MCT1/MCT4 as targets for PCa therapy., NPG received a fellowship from the Portuguese Foundation for Science and Technology (FCT), refs. SFRH/BD/61027/2009. This work was supported by the FCT grant ref. PTDC/SAUMET/113415/2009, under the scope of "Programa Operacional Tematico Factores de Competitividade" (COMPETE) of "Quadro Comunitario de Apoio III" and co-financed by Fundo Comunitario Europeu FEDER. JA was supported by a Boehringer Ingelheim Fonds fellowship.