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1. Luminal breast cancer identity is determined by loss of glucocorticoid receptor activity

Author

Stefan Prekovic, Theofilos Chalkiadakis, Merel Roest, Daniel Roden, Catrin Lutz, Karianne Schuurman, Mark Opdam, Liesbeth Hoekman, Nina Abbott, Tanja Tesselaar, Maliha Wajahat, Amy R Dwyer, Isabel Mayayo‐Peralta, Gabriela Gomez, Maarten Altelaar, Roderick Beijersbergen, Balázs Győrffy, Leonie Young, Sabine Linn, Jos Jonkers, Wayne Tilley, Theresa Hickey, Damir Vareslija, Alexander Swarbrick, and Wilbert Zwart

Subjects
breast cancer, glucocorticoids, luminal breast cancer subtypes, nuclear receptors, ZBTB16, Medicine (General), R5-920, Genetics, QH426-470
Abstract

Abstract Glucocorticoid receptor (GR) is a transcription factor that plays a crucial role in cancer biology. In this study, we utilized an in silico‐designed GR activity signature to demonstrate that GR relates to the proliferative capacity of numerous primary cancer types. In breast cancer, the GR activity status determines luminal subtype identity and has implications for patient outcomes. We reveal that GR engages with estrogen receptor (ER), leading to redistribution of ER on the chromatin. Notably, GR activation leads to upregulation of the ZBTB16 gene, encoding for a transcriptional repressor, which controls growth in ER‐positive breast cancer and associates with prognosis in luminal A patients. In relation to ZBTB16's repressive nature, GR activation leads to epigenetic remodeling and loss of histone acetylation at sites proximal to cancer‐driving genes. Based on these findings, epigenetic inhibitors reduce viability of ER‐positive breast cancer cells that display absence of GR activity. Our findings provide insights into how GR controls ER‐positive breast cancer growth and may have implications for patients' prognostication and provide novel therapeutic candidates for breast cancer treatment.

Published
2023
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2. Dynamic epi‐transcriptomic landscape mapping with disease progression in estrogen receptor‐positive breast cancer

Author

Stephen Keelan, Mihaela Ola, Sara Charmsaz, Sinéad Cocchiglia, Daniela Ottaviani, Seán Hickey, Siobhan Purcell, Fiona Bane, Aisling Hegarty, Ben Doherty, Katherine Sheehan, Lance Hudson, Nicola Cosgrove, Benjamin Roux, Muriel Laine, Geoffrey Greene, Damir Varešlija, Arnold Konrad Hill, and Leonie Young

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Published
2023
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8. Impact of the COVID-19 pandemic on cancer care in Ireland – Perspectives from a COVID-19 and Cancer Working Group

Author

Seamus O'Reilly, Hailey Kathryn Carroll, Deirdre Murray, Louise Burke, Triona McCarthy, Robert O’Connor, Claire Kilty, Sonya Lynch, Jennifer Feighan, Maeve Cloherty, Patricia Fitzpatrick, Katrina Falvey, Verena Murphy, Mary Jane O'Leary, Sophie Gregg, Leonie Young, Eilish McAuliffe, Josephine Hegarty, Anna Gavin, Mark Lawler, Paul Kavanagh, Susan Spillane, Terry McWade, Mairead Heffron, Karen Ryan, Paul J Kelly, Aileen Murphy, Mark Corrigan, H. Paul Redmond, Patrick Redmond, Paul M Walsh, Paula Tierney, Mengyang Zhang, Kathleen Bennett, and Maeve Mullooly

Subjects
Oncology, Health Policy
Published
2023
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9. An investigation of Sigma-1 receptor expression and ligand-induced endoplasmic reticulum stress in breast cancer

Author

Preeti Borde, Nicola Cosgrove, Sara Charmsaz, Stephen T. Safrany, and Leonie Young

Subjects
Cancer Research, Molecular Medicine, Molecular Biology
Abstract

Targeted therapeutic options and prognostic biomarkers for hormone receptor- or Her2 receptor-negative breast cancers are severely limited. The sigma-1 receptor, a stress-activated chaperone, is frequently dysregulated in disease. However, its significance in breast cancer (BCa) has not been adequately explored. Here, we report that the sigma-1 receptor gene (SIGMAR1) is elevated in BCa, particularly in the aggressive triple-negative (TNBC) subtype. By examining several patient datasets, we found that high expression at both the gene (SIGMAR1) and protein (Sig1R) levels associated with poor survival outcomes, specifically in ER-Her2- groups. Our data further show that high SIGMAR1 was predictive of shorter survival times in patients treated with adjuvant chemotherapy (ChT). Interestingly, in a separate cohort who received neoadjuvant taxane + anthracycline treatment, elevated SIGMAR1 associated with higher rates of pathologic complete response (pCR). Treatment with a Sig1R antagonist, 1-(4-iodophenyl)-3-(2-adamantyl)guanidine (IPAG), activated the unfolded protein response (UPR) in TNBC (high-Sig1R expressing) and ER + (low-Sig1R expressing) BCa cell lines. In tamoxifen-resistant LY2 cells, IPAG caused Sig1R to aggregate and co-localise with the stress marker BiP. These findings showcase the potential of Sig1R as a novel biomarker in TNBC as well as highlight its ligand-induced interference with the stress-coping mechanisms of BCa cells.

Published
2022

13. Physical activity and menopausal symptoms in women who have received menopause-inducing cancer treatments: results from the Women's Wellness After Cancer Program

Author

Alexandra L. McCarthy, Sarah Balaam, Tom G. Bailey, Janine Porter-Steele, Debra Anderson, Leonie Young, Gregore I. Mielke, and Tina S Skinner

Subjects
medicine.medical_specialty, Physical activity, law.invention, Blood cancer, Randomized controlled trial, law, Internal medicine, Neoplasms, medicine, Menopausal Symptom, Humans, Obstetrics & Reproductive Medicine, Generalized estimating equation, Exercise, Life Style, 11 Medical and Health Sciences, business.industry, Obstetrics and Gynecology, Cancer, medicine.disease, Menopause, Female, Self Report, Climacteric, business
Abstract

ObjectiveThis randomized controlled trial tested a digitally-delivered whole-of-lifestyle program for women previously treated for cancer. We investigated (1) associations between self-reported physical activity (PA) and menopausal symptoms and (2) if the intervention was associated with beneficial changes in PA and menopausal symptoms.MethodsWomen were randomized to intervention (n = 142) or control (n = 138). The intervention targeted lifestyle behavior including PA. Self-reported PA (International Physical Activity Questionnaire - Short Form) and menopausal symptom (Green Climacteric Scale, GCS) data were collected at baseline, with measures repeated at 12 weeks (end of intervention) and 24 weeks (to assess sustainability). Generalized estimating equation models explored associations between PA and GCS scores. Mixed-effects generalized equation models analyzed changes within and between groups in PA and GCS scores.ResultsTotal GCS scores were 1.83 (95% CI: 0.11-3.55) and 2.72 (95% CI: 1.12-4.33) points lower in women with medium and high levels of PA, respectively, than in women with low levels of PA. Total average GCS scores were 1.02 (0.21-2.26) and 1.61 (0.34-2.87) points lower in those undertaking moderate or vigorous intensity PA, respectively. Time spent walking, and performing moderate and vigorous PA were not different between intervention and control. The average GCS decrease of 0.66 points (95% CI: 0.03-1.29; p time = 0.03) over 24 weeks was not different between groups.ConclusionThis exploratory study established a stepwise association between moderate and vigorous PA and a lower total menopausal symptom score. The intervention did not appear to increase self-reported PA in women treated for early stage breast, reproductive, and blood cancers.

Published
2020

14. Facilitating lifestyle changes to manage menopausal symptoms in women with breast cancer

Author

Leonie Young, Patsy Yates, Debra Anderson, Alexandra L. McCarthy, Charrlotte Seib, Amanda McGuire, and Janine Porter-Steele

Subjects
medicine.medical_specialty, Health Behavior, Breast Neoplasms, Pilot Projects, Severity of Illness Index, law.invention, Breast cancer, Randomized controlled trial, Quality of life, law, Surveys and Questionnaires, Severity of illness, medicine, Humans, Menopausal Symptom, Life Style, Sleep disorder, business.industry, Obstetrics and Gynecology, Cancer, Middle Aged, medicine.disease, Treatment Outcome, Sexual dysfunction, Physical therapy, Female, Menopause, medicine.symptom, business
Abstract

OBJECTIVE Women diagnosed as having breast cancer may experience difficulties with posttreatment effects such as menopausal symptoms. The aims of this pilot study were to (1) evaluate the impact of a multimodal lifestyle program on reducing menopausal symptoms in women with breast cancer and (2) examine the impact of the program on health-related quality of life (HRQoL) and adherence to lifestyle recommendations. METHODS Overall, 55 women aged 45 to 60 years with one moderate to severe menopausal symptom and a history of breast cancer were randomized into an intervention group (n = 26) or a control group (n = 29). Women in the intervention group received a lifestyle intervention (The Pink Women’s Wellness Program) that included clinical consultations and a tailored health education program. Measurements of menopausal symptoms (Greene Climacteric Scale), HRQoL (SF-12 and Functional Assessment of Cancer Therapy—Breast), and modifiable lifestyle factors (food intake, physical activity, smoking and alcohol use, and sleep disturbance) were taken at baseline and 12 weeks. RESULTS Women in the intervention group reported clinically significant reductions in many menopausal symptoms, specifically somatic symptoms (d = 0.52), vasomotor symptoms (d = 0.55), sexual dysfunction (d = .65), and overall menopausal symptoms (d = 0.54), at 12 weeks compared with the control group (d = 0.03, d = 0.24, d = 0.18, and d = 0.05, respectively). Women in the intervention group reported improvements in Functional Assessment of Cancer Therapy—Breast subscale scores, physical well-being and functional well-being, and Functional Assessment of Cancer Therapy—General total scores (intervention group: d = 0.54, d = 0.50, and d = 0.48, respectively; control group: d = 0.22, d = 0.11, and d = 0.05, respectively). CONCLUSIONS The Pink Women’s Wellness Program is effective in decreasing menopausal symptoms, thus improving HRQoL. This being a pilot study, further research is recommended to investigate the benefits of combining nonpharmacological interventions for women with breast cancer to reduce their treatment-related menopausal symptoms.

Published
2015
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15. The Women's wellness after cancer program: a multisite, single-blinded, randomised controlled trial protocol

Author

Leanne Monterosso, Jane Turner, Katherine M. White, Neil A. King, Charrlotte Seib, Kathryn A. Lee, Debra Anderson, Amanda McGuire, Meinir Krishnasamy, Dian Tjondronegoro, Patsy Yates, Leonie Young, Sarah Balaam, Janine Porter-Steele, Sonja Hall, Kathy Wells, Wei Song, and Alexandra L. McCarthy

Subjects
Comparative Effectiveness Research, and promotion of well-being, Cancer Research, Evidence-based nursing, law.invention, Pittsburgh Sleep Quality Index, User-Computer Interface, 0302 clinical medicine, Randomized controlled trial, law, Neoplasms, Medicine, Modifiable lifestyle factors, 030212 general & internal medicine, Health Education, Cancer, Menopausal symptoms, 3. Good health, health-related quality of life, Oncology, 030220 oncology & carcinogenesis, Public Health and Health Services, Health education, Female, Menopause, Sleep Research, medicine.medical_specialty, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, Health Promotion, 03 medical and health sciences, Breast cancer, Quality of life (healthcare), Clinical Research, Tobacco, Breast Cancer, Behavioral and Social Science, Genetics, Humans, Women, Oncology & Carcinogenesis, Nutrition, Tobacco Smoke and Health, business.industry, Prevention, Australia, Womens Health, Evidence-Based Nursing, Prevention of disease and conditions, medicine.disease, Health Surveys, Clinical trial, Good Health and Well Being, Health promotion, Physical therapy, Quality of Life, 3.1 Primary prevention interventions to modify behaviours or promote wellbeing, Women's Health, business, New Zealand
Abstract

BackgroundDespite advances in cancer diagnosis and treatment have significantly improved survival rates, patients post-treatment-related health needs are often not adequately addressed by current health services. The aim of the Women's Wellness after Cancer Program (WWACP), which is a digitised multimodal lifestyle intervention, is to enhance health-related quality of life in women previously treated for blood, breast and gynaecological cancers.MethodsA single-blinded, multi-centre randomized controlled trial recruited a total of 351 women within 24months of completion of chemotherapy (primary or adjuvant) and/or radiotherapy. Women were randomly assigned to either usual care or intervention using computer-generated permuted-block randomisation. The intervention comprises an evidence-based interactive iBook and journal, web interface, and virtual health consultations by an experienced cancer nurse trained in the delivery of the WWACP. The 12week intervention focuses on evidence-based health education and health promotion after a cancer diagnosis. Components are drawn from the American Cancer Research Institute and the World Cancer Research Fund Guidelines (2010), incorporating promotion of physical activity, good diet, smoking cessation, reduction of alcohol intake, plus strategies for sleep and stress management. The program is based on Bandura's social cognitive theoretical framework. The primary outcome is health-related quality of life, as measured by the Functional Assessment of Cancer Therapy-General (FACT-G). Secondary outcomes are menopausal symptoms as assessed by Greene Climacteric Scale; physical activity elicited with the Physical Activity Questionnaire Short Form (IPAQ-SF); sleep measured by the Pittsburgh Sleep Quality Index; habitual dietary intake monitored with the Food Frequency Questionnaire (FFQ); alcohol intake and tobacco use measured by the Australian Health Survey and anthropometric measures including height, weight and waist-to-hip ratio. All participants were assessed with these measures at baseline (at the start of the intervention), 12weeks (at completion of the intervention), and 24weeks (to determine the level of sustained behaviour change). Further, a simultaneous cost-effectiveness evaluation will consider if the WWACP provides value for money and will be reported separately.DiscussionWomen treated for blood, breast and gynaecological cancers demonstrate increasingly good survival rates. However, they experience residual health problems that are potentially modifiable through behavioural lifestyle interventions such as the WWACP.Trial registrationThe protocol for this study was registered with the Australian and New Zealand Clinical Trials Registry, Trial ID: ACTRN12614000800628 , July 28, 2014.

Published
2017

16. Patient-Derived Xenografts of Breast Cancer

Author

Damir, Varešlija, Sinead, Cocchiglia, Christopher, Byrne, and Leonie, Young

Subjects
Disease Models, Animal, Mice, Carcinogenesis, Animals, Heterografts, Humans, Breast Neoplasms, Female, Xenograft Model Antitumor Assays
Abstract

With the advancement of translational research, particularly in the field of cancer, it is now imperative to have models which more clearly reflect patient heterogeneity. Patient derived xenograft (PDX) models, which involve the orthotopic implantation of breast tumors into immune-compromised mice, recapitulate the native tumor biology. Despite the considerable challenges that establishing PDX models present, they are the ultimate model to study tumorigenesis of refractory disease and for assessing the efficacy of new pharmaceutical compounds.

Published
2016

17. Abstracts from the 5th International Conference for Healthcare and Medical Students (ICHAMS)

Author

Yvonne Sweeney, Hugh O’Neill, Garry Duffy, Daniel Creegan, Viviana Bustos, Brian J. Harvey, Alexander Dalphy, Anthony O’Grady, Elaine Kay, Katarzyna Samelska, Justyna Izdebska, Anna Kurowska, Rena Al-Zubaidy, Magdalena Mroz, Brian Harvey, Ryan Fagan, Helen French, Vanessa Cuddy, Jennifer Ashton, Michelle Clarke, Zaid Sayedalamin, Mukhtiar Baig, Osama Almutairi, Hassan Allam, Taher F. Halawa, Hazem M. Atta, Linda Sirone, Renars Erts, Jana Pavare, Louis Richter, Joseph Morris, Irene Oglesby, Eimear Dunne, Dermot Kenny, Ibrahim Mohammed Mahdi Khayyat, Viviana Bustos Salgado, Jonavan Tan, Daragh Moneley, Austin Leahy, Patricia Fitzgerald, Evelyn Fennelly, Grace Harkin, John Lee, Erica O’Sullivan, Brian Kirby, Sarah O’Neill, Diana Gonciar, Teodora Mocan, Cristian Matea, Lucian Mocan, Cornel Iancu, Chloe Doran, Sarah Hoolahan, Tobias Engel, Maha Alkhattab, Tijna Alekseeva, William Lackington, Fergal O’Brien, Nabeehah Moollan, Noel Gerry McElvaney, Cedric Gunaratnam, Lorraine Scanlon, Noeleen Brady, Suzanne Timmons, Richard Bresler, Zita Abreu, Stefan Trohonel, Joanne Bargman, Ahmad A. Mirza, Ahmed Badrek-Amoudi, Rakan H. Aun, Hussam A. Senan, Abdulrahim A. Mirza, Mohammed S. Binsaad, Mian U. Farooq, Saheli Nandi, Beatrice D’Orsi, Jochen Prehn, Mariia Zharova, Pavel Umrukhin, Wendy Evans-Uhegbu, Frank Doyle, Hope Kudryashova, Derek Dorris, Anthony Cummins, Jemma Doheny-Shanley, Mark Woodward, Wesley Hayes, Marina Yostos, David Cotter, Melanie Focking, Samantha Stancu, Florin Iordache, Bogdan A. Popescu, Muhammad-Mujtaba A. Akanmu, Alero A. Robert, Ezekiel O. Oridota, Ali K. Alzahrani, Omar Alfarhan, Essam Nour Eldin, Bronagh MacManus, Owen Keane, Patrick Hillery, James Lee, Hugh O’Reilly, Niamh Collins, Ibrahim Abu saq, Abdullah Al Mufarrih, Muath Jaafari, Abdullah Al Mahayni, Amen Bawazir, Sultan Alkhateeb, Amenah Dhannoon, Damir Vareslija, Arnold Hill, Leonie Young, Declan Donoghue, Criona Walsh, Aileen McCabe, John Pope, Saturnino Pasco, Caroline Fallon, Don Solanki, Fiona Kiernan, Sinead Galvin, Jquan Mucvimicc, Johanna Mulvihill, Soha A. Elmosry, Lorenza Andres Ameida De Souza, Yuri de Oliveira, Diego Menezes, Alene Vanessa Santos, Ahmad Zaki Asraf, Raymond Stallings, Olga Piskareva, Ross Conlon, Siún Sweeney-Landers, Cathy Burke, Paraic Behan, Seamus Sreenan, Ahmed Organjee, Tatsiana Crosbie-Staunton, Emer Reeves, Noel McElvaney, Crystal Mieres, Sara Charmsaz, Aya Al-Jalamdeh, Mary Corcoran, Martha McElligott, Niall Stevens, Hilary Humphreys, Rashid Barnawi, Abdulaziz Ghurab, Sultan Alfaer, Hassan Balubaid, Kamal Hanbazazah, Mohammed Bukhari, Mohammed Alsakkaf, Ahmad Mirza, Amrallah Mohammed, Anastasia Pratanata, Maria Nathania, Tsabita Annisa, Beti Dewi, Kuok Zhen Lee, Tomas P. Carroll, Laura Fee, Noel G. McElvaney, Rachel C. White, and Robert T Brady

Subjects
medicine.medical_specialty, business.industry, Family medicine, Health care, polycyclic compounds, Alternative medicine, Medicine, General Medicine, Dexrazoxane, business, General Biochemistry, Genetics and Molecular Biology, medicine.drug
Abstract

O1: Assessing the protective effect of dexrazoxane against doxorubicin-induced toxicity in HL-1 cardiomyocytes

Published
2016
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18. An Evaluation ofbeyondblue, Australia's National Depression Initiative

Author

Tracey A Davenport, Leonie Young, Nicole Highet, Jane Burns, Ian B. Hickie, and Jane Pirkis

Subjects
business.industry, Health Policy, media_common.quotation_subject, Acknowledgement, Public Health, Environmental and Occupational Health, Primary care, Mental health, Literacy, Psychiatry and Mental health, Nursing, Depression (economics), Workforce, Mental health care, Medicine, business, media_common
Abstract

beyondblue is a five-year Australian initiative which takes a populationhealth approach to combating depression. This paper's aim is to describe the findings of an evaluation of beyondblue, conducted four years into its existence.The achievements of beyondblue were examined in the light of its objectives, using synthesised data from 15 secondary sources. Many of beyondblue's lower-level objectives have been completely achieved, with a plethora of key initiatives in place that have led to greater availability of information about depression, improvements in consumer networks, better support for mental health care delivery in primary care settings and increases in targeted research. Most of its intermediate-level and high-level objectives have been partly achieved, with headway made in terms of the community's ‘depression literacy’, acknowledgement of the consumer/carer perspective, the degree to which the health workforce is equipped to deal with depression, the likelihood that individuals will seek help, ...

Published
2005
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19. Enhancing community awareness of depression, access to treatment and attitudinal change: experiences from beyondblue: the national depression initiative

Author

Nicole Highet, Clare Shann, and Leonie Young

Subjects
medicine.medical_specialty, Intervention (counseling), medicine, Community awareness, Attitude change, Psychology, Psychiatry, Depression (differential diagnoses), Health care delivery
Abstract

Chapter 59 explores methods of enhancing community awareness of depression, access to treatment and attitudinal change using the example of the Australian 'bluebeyond' initiative. The initiative's aims are discussed alongside challenges that were faced and potential solutions.

Published
2010
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20. Prosaposin activates the androgen receptor and potentiates resistance to endocrine treatment in breast cancer.

Author

Ali, Azlena, Creevey, Laura, Yuan Hao, McCartan, Damian, O'Gaora, Peadar, Hill, Arnold, Leonie Young, and McIlroy, Marie

Subjects
BREAST cancer treatment, ANDROGEN receptors, GLYCOPROTEINS, GLYCOCONJUGATES, STEROID receptors
Abstract

Introduction: HOX genes play vital roles in growth and development, however, atypical redeployment of these genes is often associated with steroidal adaptability in endocrine cancers. We previously identified HOXC11 to be an indicator of poor response to hormonal therapy in breast cancer. In this study we aimed to elucidate genes regulated by HOXC11 in the endocrine resistant setting. Methods: RNA-sequencing paired with transcription factor motif-mapping was utilised to identify putative HOXC11 target genes in endocrine resistant breast cancer. Validation and functional evaluation of the target gene, prosaposin (PSAP), was performed in a panel of endocrine sensitive and resistant breast cancer cell lines. The clinical significance of this finding was explored in clinical cohorts at both mRNA and protein level. Results: PSAP was shown to be regulated by HOXC11 in both tamoxifen and aromatase inhibitor (AI) resistant cell lines. Transcript levels of HOXC11 and PSAP correlated strongly in samples of primary breast tumours (r = 0.7692, n = 51). PSAP has previously been reported to activate androgen receptor (AR) in prostate cancer cells. In a panel of breast cancer cell lines it was shown that endocrine resistant cells exhibit innately elevated levels of AR compared to their endocrine sensitive counterparts. Here, we demonstrate that stimulation with PSAP can drive AR recruitment to a hormone response element (HRE) in AI resistant breast cancer cells. Functionally, PSAP promotes cell migration and invasion only in AI resistant cells and not in their endocrine sensitive counterparts. In a cohort of breast cancer patients (n = 34), elevated serum levels of PSAP were found to associate significantly with poor response to endocrine treatment (p = 0.04). Meta-analysis of combined PSAP and AR mRNA are indicative of poor disease-free survival in endocrine treated breast cancer patients (hazard ratio (HR): 2.2, P = 0.0003, n = 661). Conclusion: The HOXC11 target gene, PSAP, is an AR activator which facilitates adaptation to a more invasive phenotype in vitro. These findings have particular relevance to the development of resistance to AI therapy which is an emerging clinical issue. PSAP is a secreted biomarker which has potential in identifying patients failing to exhibit sustained response to hormonal treatment. [ABSTRACT FROM AUTHOR]

Published
2015
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