Your search keyword '"Luke Hughes-Davies"' showing total 49 results

1. Abstract OT3-32-01: OPTIMA, a prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in high clinical risk early breast cancer

Author

Robert Stein, Andreas Makris, Iain Macpherson, Luke Hughes-Davies, Andrea Marshall, Georgina Dotchin, David A. Cameron, Belinda E. Kiely, Caroline Wilson, Anne Armstrong, Helena M. Earl, Christopher J. Poole, Janice Tsang, Bjørn Naume, Daniel Rea, Hege Ohnstad, Peter S. Hall, Stuart A. McIntosh, Bethany Shinkins, Christopher McCabe, Adrienne Morgan, John MS Bartlett, and Janet A. Dunn

Subjects

Cancer Research, Oncology

Abstract

Background: Multi-parameter tumor gene expression assays (MPAs) are used to estimate individual patient risk and guide chemotherapy use in hormone-sensitive, HER2-negative early breast cancer. The TAILORx trial supports MPA use in a node-negative population. Evidence for MPA use in postmenopausal node-positive breast cancer has been provided by the RxPONDER trial interim analysis but this relies on the absence of superiority in an analysis where >50% of events were unrelated to breast cancer. There is much uncertainty about MPA use for premenopausal patients. OPTIMA (Optimal Personalised Treatment of early breast cancer usIng Multi-parameter Analysis) (ISRCTN42400492) is a prospective international randomized controlled trial designed to validate MPAs as predictors of chemotherapy sensitivity in a largely node-positive breast cancer population. Methods: OPTIMA is a partially blinded study with an adaptive two-stage design. The trial recruits women and men age 40 or older with resected ER-positive, HER2-negative invasive breast cancer and up to 9 involved axillary lymph nodes. Randomization is to standard management (chemotherapy and endocrine therapy) or to MPA-directed treatment using the Prosigna (PAM50) test. Those with a Prosigna tumor Score (ROR_PT) >60 receive standard management whilst those with a low score (≤60) tumor are treated with endocrine therapy alone. Endocrine therapy for pre-menopausal women includes ovarian suppression for all participants unless they experience a chemotherapy-induced menopause. Adjuvant abemaciclib is permitted. The trial will be analyzed for (1) non-inferiority of recurrence according to randomization and (2) cost-effectiveness. The key secondary outcome is non-inferiority of recurrence for patients with low ROR_PT score tumors. The efficacy analyses will be performed Per Protocol using Invasive Breast Cancer Free Survival (IBCFS) as the primary outcome measure to limit the risk of a false non-inferiority conclusion. Recruitment of 4500 patients over 8 years will permit demonstration of up to 3% non-inferiority of test-directed treatment with at least 83% power, assuming 5-year IBCFS is 87% with standard management. An integrated qualitative recruitment study addresses challenges to consent and recruitment, building on experience from the feasibility study which found that a multidisciplinary approach is important for recruitment success. OPTIMA is strongly supported by a patient group which has helped design all patient documents and which is represented on the TMG. Results: The OPTIMA main trial opened in January 2017 and has continued to recruit throughout the COVID-19 pandemic. Overall recruitment as of 1 July 2022 was 2814 (2593 from UK, 221 from Norway). Patient characteristics are well balanced between the trial arms. Currently 95% of randomized participants are eligible for inclusion in the PP analysis. 66% of the MPA-directed arm participants have been allocated to endocrine therapy only. The test failure rate is < 1%. Conclusion: OPTIMA will provide robust unbiased evidence on test-directed chemotherapy safety for both postmenopausal and premenopausal women with 1-3 involved nodes as well as for patients with 4-9 involved nodes and for patients treated with abemaciclib. Funding: OPTIMA is funded by the UK NIHR HTA Programme (10/34/501) and in Norway by KLINBEFORSK and the Norwegian Cancer Society. Views expressed are those of the authors and not those of the HTA Programme, NIHR, NHS or the Department of Health. Trial Inquiries: OPTIMA@warwick.ac.uk Patient characteristics Citation Format: Robert Stein, Andreas Makris, Iain Macpherson, Luke Hughes-Davies, Andrea Marshall, Georgina Dotchin, David A. Cameron, Belinda E. Kiely, Caroline Wilson, Anne Armstrong, Helena M. Earl, Christopher J. Poole, Janice Tsang, Bjørn Naume, Daniel Rea, Hege Ohnstad, Peter S. Hall, Stuart A. McIntosh, Bethany Shinkins, Christopher McCabe, Adrienne Morgan, John MS Bartlett, Janet A. Dunn. OPTIMA, a prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in high clinical risk early breast cancer. [abstract]. In: Proceedings of the 2022 San Antonio Breast Cancer Symposium; 2022 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2023;83(5 Suppl):Abstract nr OT3-32-01.

Published

2023

2. Definition of Tumor Bed Boost in Oncoplastic Breast Surgery: An Understanding and Approach

Author

Amit Agrawal, Sara Lightowlers, Luke Hughes-Davies, E. Garreffa, and Simon Russell

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Mammaplasty, medicine.medical_treatment, Breast surgery, Breast Neoplasms, Mastectomy, Segmental, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Fiducial Markers, Breast-conserving surgery, medicine, Humans, Breast, Cooperative Behavior, CLIPS, Radiation oncologist, Retrospective Studies, computer.programming_language, Surgeons, Contouring, business.industry, Radiotherapy Planning, Computer-Assisted, Radiation Oncologists, Dose-Response Relationship, Radiation, Radiotherapy Dosage, medicine.disease, Tumor Burden, Radiation therapy, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Female, Radiotherapy, Adjuvant, Radiology, Tomography, X-Ray Computed, business, Perforator Flap, computer, Perforator flaps

Abstract

Introduction Definition of the tumor bed (TB) is currently guided by intraoperatively placed metal clips. However, this traditional planning method may not be sufficient for tumor cavity defect refilled with modern oncoplastic breast surgery. We explored the impact of a close cooperation between surgeon and oncologist on the accuracy of TB contouring after partial breast reconstruction with chest wall perforator flaps (CWPF). Patients and Methods A retrospective review of patients who received radiotherapy after CWPF was performed. TB and boost volume were defined by the surgeon, considering clips and the typical radiologic appearance of the flap, and by a radiation oncologist, and results were compared with the surgical specimen volume (SPV). The boost volume was marked as 5 mm penumbral ring thickness of native breast tissue wall around the replaced flap (nonbreast tissue). Results There were no significant differences between SPV and surgeon-defined TB values. Conversely, the radiation oncologist–defined values were significantly smaller than the actual SPV. If a ring-shaped TB boost was delivered, this would have allowed a potential reduction of irradiated tissue of 127.6%. Conclusion TB definition solely by surgical clips may be prone to inaccuracy in case of volume replacement oncoplastic breast surgery. Our approach of combining the clips with the redefinition of the flap on computed tomographic scan may provide more accurate TB definition. Although an ideal ring-shaped boost might be difficult to reproduce in practice, it introduces a new paradigm: a lower radiation dose inside TB is tolerable, if not desirable, at least in CWPF.

Published

2020

3. Abstract OT3-17-01: OPTIMA: A prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in mostly node-positive early breast cancer

Author

Victoria Harmer, Jenny L Donovan, Daniel Rea, Christopher McCabe, Luke Hughes-Davies, Stuart McIntosh, Peter Hall, Adrienne Morgan, David Cameron, Andrea Marshall, Bethany Shinkins, Christopher J. Poole, John M. S. Bartlett, Iain R. Macpherson, Robert Stein, Andreas Makris, Sarah E Pinder, Leila Rooshenas, Abeer M Shaaban, Helena M. Earl, Nigel Stallard, Janet A. Dunn, Georgina Dotchin, Carmel Conefrey, and Bjørn Naume

Subjects

Cancer Research, medicine.medical_specialty, education.field_of_study, Axillary lymph nodes, business.industry, Cost effectiveness, Population, Cancer, medicine.disease, law.invention, Breast cancer, medicine.anatomical_structure, Oncology, Quality of life, Randomized controlled trial, law, Interquartile range, Internal medicine, medicine, business, education

Abstract

Background: Multi-parameter tumour gene expression assays (MPAs) are widely used to estimate individual patient risk and to guide chemotherapy use in hormone-sensitive, HER2-negative early breast cancer. The TAILORx trial supports MPA use in a node-negative population. Evidence in node-positive breast cancer is limited. OPTIMA (Optimal Personalised Treatment of early breast cancer usIng Multi-parameter Analysis) (ISRCTN42400492) is a prospective international randomised controlled trial (RCT) designed to validate MPA’s as predictors of chemotherapy sensitivity in a largely node-positive breast cancer population. Methods: OPTIMA is a partially blinded study with an adaptive two-stage design. The main eligibility criteria are women and men age 40 or older with resected ER-positive, HER2-negative invasive breast cancer and up to 9 involved axillary lymph nodes. Randomisation is to standard management (chemotherapy and endocrine therapy) or to MPA-directed treatment using the Prosigna (PAM50) test. Those with a Prosigna tumour Score (ROR_PT) >60 receive standard management whilst those with a low score (≤60) are treated with endocrine therapy alone. Endocrine therapy for pre-menopausal women includes ovarian suppression. Prosigna tests are currently performed only for participants randomised to MPA-directed treatment. More than 1 tumour may be tested if participants have multi-focal tumours with discordant features and/or are considered clinically significant. The co-primary outcomes are: (1) Invasive Disease Free Survival (IDFS) and (2) cost-effectiveness. Secondary outcomes include IDFS in patients with low-score tumours and quality of life. Recruitment of 4500 patients over 5 years will permit demonstration of 3% non-inferiority of test-directed treatment, assuming 5-year IDFS of 85% with standard management. An integrated qualitative recruitment study addresses challenges to consent and recruitment, building on experience from the feasibility study which found that a multidisciplinary approach is important for recruitment success. Results: The OPTIMA main trial opened in January 2017. Overall recruitment as of 1 July 2019 was 1123 (1100 from UK, 13 from Norway); 91% had axillary node macro-metastases. Median time from consent to treatment allocation was 12 days (interquartile range 10-14 days). The withdrawal rate from trial treatment is 3%; 50% of these continue with follow up. Prosigna tests have been performed on 608 tumours for 549 participants; 59% were luminal A, 38% were luminal B and 3% non-luminal (6 patients with non-luminal tumours [1% overall] were ineligible on receptor retesting). Of the 53 (10%) participants with >1 tumour tested, 3 (6%) had discordant scores only, 7 (13%) had discordant subtypes only and 8 (15%) had both discordant scores and subtypes. Two thirds of the MPA-directed arm participants have been allocated to endocrine therapy only. The test failure rate is Conclusion: OPTIMA is one of two large scale prospective trials validating the use of test-guided chemotherapy decisions in node-positive early breast cancer. It is expected to have a global impact on breast cancer treatment. Funding: OPTIMA is funded by the UK NIHR HTA Programme (10/34/501). Views expressed are those of the authors and not those of the HTA Programme, NIHR, NHS or the Department of Health. Trial Inquiries: OPTIMA@warwick.ac.uk Citation Format: Robert C Stein, Andrea Marshall, Andreas Makris, Luke Hughes-Davies, Iain R MacPherson, Carmel Conefrey, Leila Rooshenas, Sarah E Pinder, Abeer M Shaaban, Bjørn Naume, David A Cameron, Daniel W Rea, Helena M Earl, Christopher J Poole, Peter S Hall, Georgina Dotchin, Stuart A McIntosh, Victoria Harmer, Adrienne Morgan, Bethany Shinkins, Nigel Stallard, Christopher McCabe, Jenny L Donovan, John MS Bartlett, Janet A Dunn. OPTIMA: A prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in mostly node-positive early breast cancer [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr OT3-17-01.

Published

2020

4. Abstract P3-10-05: Preliminary safety data from stage 1 and 2 of the phase II/III PARTNER trial: Addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients

Author

Luke Hughes-Davies, Ellen Copson, Bryony Harrop, Karen Pinilla Alba, Paula del Rosario, Anne C Armstrong, Nikolaos Demiris, R Roylance, Emma McMurtry, L Grybowicz, Wendi Qian, Caron Harvey, Marc Tischkowitz, Karen McAdam, Elena Provenzano, Anne-Laure Vallier, Helena M. Earl, Stanly Thomas, and Jean Abraham

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Population, Neutropenia, Olaparib, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, Internal medicine, medicine, education, education.field_of_study, business.industry, Cancer, medicine.disease, Carboplatin, Regimen, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, business, Febrile neutropenia

Abstract

Background: Triple negative breast cancers (TNBCs) are an aggressive and diverse subgroup with no specific targeted therapies currently available. Basal TNBCs show some phenotypic and molecular similarities with germline BRCA mutated BC (gBRCA). In gBRCA patients, and potentially other homologous recombination deficiencies, these already compromised pathways may allow PARP inhibitors (olaparib) to work more effectively. PARTNER was designed to establish if the addition of olaparib to neoadjuvant platinum-based chemotherapy for gBRCA and/or basal TNBC is safe and improves efficacy (pathological complete response (pCR)). This is the first time a clinical trial provides safety data of the combination of olaparib with platinum and taxane chemotherapy in an early breast cancer setting. Methods: PARTNER is a 3-stage open label randomised Phase II/III trial of neoadjuvant Carboplatin AUC5 with weekly Paclitaxel 80mg/m2 (CP) +/- olaparib (O) 150mgBD for 12 days x 4 cycles, followed by clinicians' choice of anthracycline regimen x 3 cycles. Basal-TNBC and/or gBRCA patients are eligible for inclusion. Primary endpoints are defined by stage: Stage 1 - Safety, Stage2 - Schedule selection, and Stage 3 - Efficacy (pCR rate). The trial is now powered for efficacy analysis in the BRCA and non-BRCA population independently. Stage 1 and 2 randomization was(1:1:1) to CP: CP + O from day (D) -2: or CP + O from D 3. G-CSF was mandatory during the first 4 cycles of treatment. We present a pooled-safety analysis from Stage 1 and 2 of the two research arms only. Recruitment continues into Stage 3. Results: Between June 2016 and April 2018, 159 patients were recruited among the three arms. Overall, median age was 48.2 [range 22.3- 70.9]; 12% had Tumours >5cm, 34% had Axillary involvement; 17% were gBRCA. Adverse events (AE) that were reported as common (in at least 10% of patients) were Anaemia 23%, Neutropenia 18% and Infection 10%. Fatigue and Diarrhoea were next most prevalent with 9% and 6% respectively. The most common AE Grade >=3 were haematological events. These include Neutropenia 19%, Anaemia 15%, and Thrombocytopenia 5%. Febrile Neutropenia and Haemorrhage were reported in only 2% and 1% of cases. Grade 3 Non- haematological events were Fatigue 7%, Hypertension 3%, Headache 3% and Diarrhoea 2%. Grade 3 Sensory neuropathy was present in 2% of patients. No grade 4 sensory or motor neuropathy events were described. Serious adverse reactions related to investigational regimen were reported in 17% of patients and include fever and infection with 8 and 4 events respectively. No toxicity related deaths were reported. As per July 8th 2019, 373 patients have been recruited from which 58 were gBRCA. Conclusions: Combinations of olaparib with neoadjuvant CP chemotherapy showed an acceptable and manageable toxicity profile. Although haematological events were the most common, they did not exceed historical frequencies reported for standard chemotherapy regimens. Final safety analysis will be performed once recruitment is complete and will include detailed long-term neuropathy data. Citation Format: Karen Pinilla Alba, Emma McMurtry, Anne-Laure Vallier, Louise Grybowicz, Ellen Copson, Anne Armstrong, Rebecca Roylance, Wendi Qian, Nikolaos Demiris, Stanly Thomas, Caron Harvey, Luke Hughes-Davies, Karen McAdam, Paula del Rosario, Bryony Harrop, Elena Provenzano, Marc Tischkowitz, Helena M Earl, Jean E Abraham. Preliminary safety data from stage 1 and 2 of the phase II/III PARTNER trial: Addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P3-10-05.

Published

2020

5. Abstract OT1-05-02: OPTIMA: A prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in high clinical risk early breast cancer

Author

Helen B Higgins, Christopher J. Poole, Christopher McCabe, Victoria Harmer, Iain R. Macpherson, Jms Bartlett, Andreas Makris, SA MacIntosh, Robert Stein, D.W. Rea, Sarah E Pinder, H. M. Earl, James D. Thomas, Leila Rooshenas, Jenny L Donovan, Luke Hughes-Davies, David Cameron, Claire Hulme, Andrea Marshall, Peter Hall, Nigel Stallard, Adrienne Morgan, Bjørn Naume, Janet A. Dunn, and Carmel Conefrey

Subjects

Oncology, Cancer Research, education.field_of_study, medicine.medical_specialty, Axillary lymph nodes, business.industry, Cost effectiveness, Population, Cancer, medicine.disease, law.invention, Residual risk, Breast cancer, medicine.anatomical_structure, Randomized controlled trial, Quality of life, law, Internal medicine, medicine, education, business

Abstract

Background:Multi-parameter tumour gene expression assays (MPAs) are widely used to estimate individual patient residual risk and to guide chemotherapy use in hormone-sensitive, HER2-negative early breast cancer. The TAILORx trial supports MPA use in a node-negative population. Evidence for MPA use in node-positive breast cancer is limited. OPTIMA (Optimal Personalised Treatment of early breast cancer usIng Multi-parameter Analysis) (ISRCTN42400492) aims to validate MPAs as predictors of chemotherapy sensitivity in a largely node-positive breast cancer population where prospective RCT (Randomised Controlled Trial) evidence is lacking. Methods: OPTIMA is a partially blinded multi-center RCT with an adaptive two-stage design. The main eligibility criteria are women and men age 40 or older with resected ER-positive, HER2-negative invasive breast cancer and up to 9 involved axillary lymph nodes. Randomisation is to standard management (chemotherapy and endocrine therapy) or to MPA-directed treatment using the Prosigna (PAM50) test. Those with a Prosigna tumour score (ROR_PT) >60 receive standard management whilst those with a low score (≤60) are treated with endocrine therapy alone. Endocrine therapy for pre-menopausal women includes ovarian suppression. The co-primary outcomes are (1) Invasive Disease Free Survival (IDFS) and (2) cost-effectiveness of test-directed treatment. Secondary outcomes include IDFS in patients with low-score tumours and quality of life. An integrated qualitative recruitment study addresses challenges to consent and recruitment and will build on experience from the feasibility study that a multidisciplinary approach at sites is important for recruitment success. Tumour blocks will be banked to allow evaluation of additional MPA technologies. Recruitment of 4500 patients over 5 years will permit demonstration of 3% non-inferiority of test-directed treatment, assuming 5-year IDFS of 85% with standard management, equivalent to a HR of 1.22. Inclusion of patients from the feasibility study will increase the power to test for non-inferiority. Results: The OPTIMA main trial opened in January 2017. Overall recruitment (including the feasibility study) will reach 1000 in August 2018. Recruitment in Norway will commence in July 2018. Characteristics of the OPTIMA main participants recruited to 31st May 2018 are shown in the table. Main study patient characteristicsCharacteristic %Median age in years (range)57 (40-80) Menopause statusPre34 Post66 Male1Tumour size=30mm42Node statuspN04 pN1mi(sn)7 pN1(sn)20 pN155 pN214Historic grade16 258 336 Conclusion: OPTIMA is one of two large scale prospective trials validating the use of test-guided chemotherapy decisions in node-positive early breast cancer. It is expected to have a global impact on breast cancer treatment. Experience from the preliminary study and close engagement with centres will aid trial success. Funding: OPTIMA is funded by the UK NIHR HTA Programme (10/34/501). Views expressed are those of the authors and not those of the HTA Programme, NIHR, NHS or the DoH. Citation Format: Stein RC, Hughes-Davies L, Makris A, Macpherson IR, Conefrey C, Rooshenas L, Pinder SE, Thomas J, Hall PS, Cameron DA, Earl HM, Naume B, Poole CJ, Rea DW, MacIntosh SA, Harmer V, Morgan A, Hulme C, McCabe C, Stallard N, Higgins H, Donovan JL, Bartlett JM, Marshall A, Dunn JA. OPTIMA: A prospective randomized trial to validate the clinical utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in high clinical risk early breast cancer [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr OT1-05-02.

Published

2019

6. Optimising the duration of adjuvant trastuzumab in early breast cancer in the UK

Author

Maggie Wilcox, Luke Hughes-Davies, Peter Hall, David Cameron, Jean Abraham, Daniel Rea, Iain R. Macpherson, E. O'Riordan, Helena M. Earl, Carlos Caldas, Sophie Gasson, Andrew M Wardley, Duncan Wheatley, David Miles, Janine Mansi, Louise Hiller, Janet A. Dunn, Karen McAdam, Earl, Helena [0000-0003-1549-8094], Abraham, Jean [0000-0003-0688-4807], Caldas, Carlos [0000-0003-3547-1489], and Apollo - University of Cambridge Repository

Subjects

medicine.medical_specialty, business.industry, MEDLINE, Nice, Cancer, 32 Biomedical and Clinical Sciences, 3211 Oncology and Carcinogenesis, medicine.disease, Lower risk, Article, RC0254, Oncology, Trastuzumab, Internal medicine, Neratinib, medicine, Radiology, Nuclear Medicine and imaging, Pertuzumab, business, Survival rate, computer, medicine.drug, computer.programming_language

Abstract

Adjuvant trastuzumab for patients with HER2-positive early breast cancer showed significant improvements in both disease-free and overall survival with 12 months of treatment [1,2], which was approved by the National Institute for Health and Care Excellence (NICE) in the UK in 2006. When the FinHer trial showed similar results with 9 weeks of trastuzumab [3], there was significant interest in whether shorter durations might be as effective. Additional benefits for patients could be less toxicity, fewer hospital visits and a more rapid return to normal life, with considerable societal benefits of reduced costs. PERSEPHONE was the pragmatic UK duration trial funded by the National Institute for Health Research, Health Technology Assessment Programme (NIHR HTA), which showed that 6 months of adjuvant trastuzumab was non-inferior to 12 months with a 4-year disease-free survival rate of 89.4% compared with 89.8% (non-inferiority P = 0.01) [4]. Less toxicity was reported with 6 months, particularly cardiac toxicity, and there were cost savings over the first 2 years [5], which were maintained over an average patient's lifetime when extrapolated using an economic model. After the publication of these results in June 2019, the Optimal Duration of Adjuvant Trastuzumab Working Group was convened, comprising a diverse, multidisciplinary membership. There were representatives from the PERSEPHONE Trial Management Group, including patient advocates, the National Cancer Research Institute (NCRI) Breast Group, the Association of Cancer Physicians, the Royal College of Radiologists and the Independent Cancer Patients' Voice. By November 2019, both dual antibody treatment with trastuzumab and pertuzumab [6] and extended neratinib after single-agent trastuzumab [7] had been approved by NICE, only for those at high risk of recurrence. Therefore, single-agent trastuzumab remained standard of care for those at lower risk of recurrence and recommendations were made for these patients.\ud \ud

Published

2021

7. Abstract OT1-06-01: OPTIMA: A prospective randomized trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in early breast cancer

Author

Iain R. Macpherson, Jms Bartlett, Leila Rooshenas, Peter Hall, Janet A. Dunn, Robert Stein, Carmel Conefrey, Jenny L Donovan, Christopher J. Poole, Stuart McIntosh, Aideen Campbell, Andrea Marshall, Helen B Higgins, Claire Hulme, Andreas Makris, D.W. Rea, Luke Hughes-Davies, David Cameron, H. M. Earl, Sarah E Pinder, Christopher McCabe, Adrienne Morgan, Victoria Harmer, and Nigel Stallard

Subjects

Oncology, Cancer Research, education.field_of_study, medicine.medical_specialty, Axillary lymph nodes, medicine.diagnostic_test, Cost effectiveness, business.industry, Population, Cancer, medicine.disease, law.invention, medicine.anatomical_structure, Breast cancer, Randomized controlled trial, Quality of life, law, Internal medicine, medicine, education, Oncotype DX, business

Abstract

Background: Multi-parameter gene expression assays (MPAs) are widely used to estimate individual patient residual risk in hormone-sensitive HER2-negative node-negative early breast cancer, allowing patients with low risk to safely avoid chemotherapy. Evidence for MPA use in node-positive breast cancer is limited. OPTIMA (Optimal Personalised Treatment of early breast cancer usIng Multi-parameter Analysis) aims to validate MPA's as predictors of chemotherapy sensitivity in a largely node-positive breast cancer population. Methods: OPTIMA is a partially blinded multi-center, phase 3 randomized controlled trial with an adaptive two-stage design. The main eligibility criteria are women or men aged 40 or older with resected ER-positive, HER2-negative breast cancer and up to 9 involved axillary lymph nodes. Randomization is to standard management (chemotherapy and endocrine therapy) or to MPA-directed treatment. Those with a “high risk” tumor MPA score receive standard management whilst those at “low risk” are treated with endocrine therapy alone. The preliminary phase (OPTIMA prelim) evaluated the performance of several MPAs to select a test to be used in the main efficacy trial based on economic analysis, and assessed the feasibility and acceptability of a large UK trial. OPTIMA prelim used Oncotype DX as the primary discriminator; the main trial will use Prosigna (PAM50) with Prosigna Score ≤60 defined as “low-risk”. The co-primary outcomes are (1) Invasive Disease Free Survival (IDFS) and (2) cost-effectiveness of test-directed therapy. Secondary outcomes include IDFS in “low-risk” patients, quality of life and additional survival measures. An integrated qualitative recruitment study will identify and address challenges to recruitment and informed consent. Tumor blocks from all consenting participants will be banked allowing the performance of alternative MPA technologies to be evaluated. Recruitment of 4500 patients will permit demonstration of 3% non-inferiority of test-directed treatment, with 5% significance and 85% power, assuming 3 years follow-up and a control arm 5-year IDFS of at least 85%. The addition of patients from OPTIMA prelim will allow non-inferiority to be assessed with 2.5% significance. Results: OPTIMA-prelim recruited 412 patients in 23 months from 35 sites with a 47% acceptance rate. The main study opened in January 2017. Early progress indicates that the recruitment target is achievable in the intended 46-month timescale through the participation of >100 sites Conclusion: OPTIMA, as one of two large scale prospective trials validating the use of test-guided chemotherapy decisions in node-positive early breast cancer, is expected to have a global impact on breast cancer treatment. Experience from OPTIMA prelim showed that patient advocate support and close engagement with sites will aid trial success. Funding: The project is funded in the UK by the NIHR HTA Programme (10/34/501). Views expressed are those of the authors and not those of the HTA Programme, NIHR, NHS or the DoH. Citation Format: Stein RC, Makris A, Hughes-Davies L, Macpherson IR, Hall PS, Cameron DA, Earl HM, Pinder SE, Poole CJ, Rea DW, McIntosh S, Harmer V, Morgan A, Rooshenas L, Conefrey C, Donovan JL, Hulme C, McCabe C, Stallard N, Campbell A, Higgins H, Bartlett JMS, Marshall A, Dunn JA. OPTIMA: A prospective randomized trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions in early breast cancer [abstract]. In: Proceedings of the 2017 San Antonio Breast Cancer Symposium; 2017 Dec 5-9; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2018;78(4 Suppl):Abstract nr OT1-06-01.

Published

2018

8. 6 versus 12 months of adjuvant trastuzumab for HER2-positive early breast cancer (PERSEPHONE) : 4-year disease-free survival results of a randomised phase 3 non-inferiority trial

Author

Jane Brown, Roshan Agarwal, Catherine Harper-Wynne, A. Humphreys, Eliot Sims, Peter Hall, Mukesh Mukesh, Sundus Yahya, Nawaz Walji, Mojca Persic, Donna L. Howe, Simon Waters, Wendy Taylor, Anita Chhabra, Karen Tipples, Helen Innes, Mark Churn, Peter Ostler, Pamela Woodings, Helen Roe, Lisa H Barraclough, Shrushma Loi, Maggie Wilcox, Susan Lupton, Adrian Harnett, Rebecca Bowen, Peter Simmonds, Natasha Mithal, H. M. Earl, Apurna Jegannathen, Kathryn Wright, A.S. Dhadda, Rozenn Allerton, Jean Abraham, Karen McAdam, Ioannis Gounaris, Mohini Varughese, Mark Harries, Helen Neville-Webbe, Catherine Bale, Narottam Thanvi, Carolyn Bedi, Carlos Caldas, Fharat A. Raja, Helena M. Earl, David Miles, Trevor McGolick, Andrew D. Goodman, Kerry Raynes, Anthony Neal, Richard Simcock, Hartmut Kristeleit, Carol MacGregor, Christopher McCabe, Caroline Archer, Laura Pettit, Chris Bradley, Anne-Laure Vallier, Urmila Barthakur, Perric Crellin, S O'Reilly, Betania Mahler Araujo, Andrew Eichholz, Louise Hiller, Anne Rigg, Janine Mansi, Jacqueline Newby, Janet A. Dunn, Sarah Smith, Chris Plummer, Jennifer Marshall, Aian Moss, Zafar Malik, Larry Hayward, Mohammad Butt, Andrew M Wardley, Anup Vinayan, Shiroma De Silva-Minor, Mei-Lin Ah-See, Sue Down, Helen B Higgins, Catherine Reed, Kim Benstead, Rakesh Mehra, Luke Hughes-Davies, David Cameron, Daniel Nelmes, O.S. Din, Charlotte Moss, Daniel Epurescu, Anne C Armstrong, Nicola Storey, David J. Eaton, Hafiz Algurafi, Mariam Jafri, Daniel Rea, Nihal Shah, Elena Provenzano, Susan Cleator, Muireann Kelleher, Claire Hulme, Daniela Lee, D. Bloomfield, Margaret Daly, Joanne Cliff, Chee Goh, Sanjay Raj, Maher Hadaki, Jayant S. Vaidya, Robert Grieve, and PERSEPHONE Steering Committee and Trial Investigators

Subjects

Oncology, medicine.medical_specialty, medicine.medical_treatment, Breast Neoplasms, 030204 cardiovascular system & hematology, Article, Disease-Free Survival, RC0254, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Adjuvants, Immunologic, Trastuzumab, Internal medicine, medicine, Adjuvant therapy, Humans, 030212 general & internal medicine, Young adult, Prospective cohort study, Adjuvants, Pharmaceutic, Early breast cancer, Chemotherapy, business.industry, General Medicine, medicine.disease, business, Adjuvant, medicine.drug

Abstract

Background: Adjuvant trastuzumab significantly improves outcomes for patients with HER2-positive early breast cancer. The standard treatment duration is 12 months but shorter treatment could provide similar efficacy while reducing toxicities and cost. We aimed to investigate whether 6-month adjuvant trastuzumab treatment is non-inferior to the standard 12-month treatment regarding disease-free survival.Methods: This study is an open-label, randomised phase 3 non-inferiority trial. Patients were recruited from 152 centres in the UK. We randomly assigned patients with HER2-positive early breast cancer, aged 18 years or older, and with a clear indication for chemotherapy, by a computerised minimisation process (1:1), to receive either 6-month or 12-month trastuzumab delivered every 3 weeks intravenously (loading dose of 8 mg/kg followed by maintenance doses of 6 mg/kg) or subcutaneously (600 mg), given in combination with chemotherapy (concurrently or sequentially). The primary endpoint was disease-free survival, analysed by intention to treat, with a non-inferiority margin of 3% for 4-year disease-free survival. Safety was analysed in all patients who received trastuzumab. This trial is registered with EudraCT (number 2006–007018–39), ISRCTN (number 52968807), and ClinicalTrials.gov (number NCT00712140).Findings: Between Oct 4, 2007, and July 31, 2015, 2045 patients were assigned to 12-month trastuzumab treatment and 2044 to 6-month treatment (one patient was excluded because they were double randomised). Median follow-up was 5·4 years (IQR 3·6–6·7) for both treatment groups, during which a disease-free survival event occurred in 265 (13%) of 2043 patients in the 6-month group and 247 (12%) of 2045 patients in the 12-month group. 4-year disease-free survival was 89·4% (95% CI 87·9–90·7) in the 6-month group and 89·8% (88·3–91·1) in the 12-month group (hazard ratio 1·07 [90% CI 0·93–1·24], non-inferiority p=0·011), showing non-inferiority of the 6-month treatment. 6-month trastuzumab treatment resulted in fewer patients reporting severe adverse events (373 [19%] of 1939 patients vs 459 [24%] of 1894 patients, p=0·0002) or stopping early because of cardiotoxicity (61 [3%] of 1939 patients vs 146 [8%] of 1894 patients, pInterpretation: We have shown that 6-month trastuzumab treatment is non-inferior to 12-month treatment in patients with HER2-positive early breast cancer, with less cardiotoxicity and fewer severe adverse events. These results support consideration of reduced duration trastuzumab for women at similar risk of recurrence as to those included in the trial.Funding: UK National Institute for Health Research, Health Technology Assessment Programme.

Published

2019

9. Optima: Optimal personalised treatment of early breast cancer using multi-parameter analysis, an international randomized trial of tumor gene expression test-directed chemotherapy treatment in a largely node-positive population

Author

Iain R. Macpherson, Robert Stein, Peter Hall, Janice Tsang, Daniel Rea, Hege O. Ohnstad, Andrea Marshall, Georgina Dotchin, Bjørn Naume, Luke Hughes-Davies, Adrienne Morgan, John M. S. Bartlett, Janet A. Dunn, David Cameron, Andreas Makris, Belinda E Kiely, Christopher McCabe, Stuart McIntosh, and Bethany Shinkins

Subjects

Oncology, Cancer Research, Chemotherapy, medicine.medical_specialty, education.field_of_study, business.industry, Adjuvant chemotherapy, medicine.medical_treatment, Population, law.invention, Randomized controlled trial, law, Internal medicine, Gene expression, Medicine, business, education, Multi parameter, Early breast cancer

Abstract

TPS599 Background: Multi-parameter tumor gene expression assays (MPAs) are validated tools to assist adjuvant chemotherapy decisions for post-menopausal women with luminal-type node-negative breast cancer. Currently there is less certainty for women with 1-3 involved axillary lymph nodes and no information on MPA use for patients with higher level nodal involvement. Three RCTs with available data report chemotherapy benefit for premenopausal women; with limited use of ovarian function suppression (OFS) for non-chemotherapy treated participants, chemotherapy-induced menopause may explain these results. Methods: OPTIMA is an international academic, partially-blinded RCT of test-directed chemotherapy treatment with an adaptive design. Women and men aged 40 or older with resected luminal-type breast cancer may participate if they fulfil one of the following stage criteria: pN1-2; pN1mi with pT ≥20mm; pN0 with pT ≥30mm. Consenting patients are randomized between standard treatment with chemotherapy followed by endocrine therapy or to undergo Prosigna testing; those with high-Prosigna Score ( > 60) tumors receive standard treatment whilst those with low-score tumors are treated with endocrine therapy alone. Patients are informed only of their treatment; test details, and randomization for chemotherapy-treated patients are masked. Clinical choice of chemotherapy is declared at randomization from a menu of standard regimens. Endocrine therapy must be for at least 5 years. Women postmenopausal at trial entry should receive an AI; men, tamoxifen; and premenopausal women, either an AI or tamoxifen, and OFS for 3 or more years; OFS initiation may be deferred because of post-chemotherapy amenorrhea. OPTIMA aims to randomize 2250 patients in each arm to demonstrate non-inferiority of test directed treatment, defined as not more than 3% below the estimated 85% 5-year IDFS for the control arm with a one sided 5% significance level. Power is 81% assuming recruitment over 96-months from January 2017 and 12 months minimum follow-up. OPTIMA also has at least 80% power to demonstrate 3.5% non-inferiority of IDFS for patients with low Prosigna Score tumors (estimated 65% of participants). Cox proportional hazards models will be used to explore important prognostic factors including menopausal status. Additional secondary endpoints include DRFI. A cost-effectiveness analysis of protocol specified MPA driven treatment against standard clinical practice will be conducted. At 31/01/2021, 2004 patients had been randomized. The DMC reviewed the trial in December 2020 with knowledge of related trial results and suggested that the trial continues as planned. OPTIMA is registered as ISRCTN42400492 and funded by the UK NIHR Health Technology Assessment Programme, award number 10/34/501. Clinical trial information: ISRCTN42400492.

Published

2021

10. Should chemotherapy in neoadjuvant setting in node positive breast cancers be guided by biology over magnitude of tumour burden?

Author

P. Forouhi, K. McAdam, V. Psychogiou, Luke Hughes-Davies, E. Garreffa, Elena Provenzano, Amit Agrawal, John R. Benson, A. Newton, P. Wignarajah, Stephen J. Russell, Charles Wilson, and N. Borkar

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Node (networking), medicine.medical_treatment, Internal medicine, medicine, Biology

Published

2020

11. Abstract P4-11-07: Comparison of multiparameter tests in the UK OPTIMA-Prelim trial

Author

Amy F Campbell, Christopher J. Poole, John M. S. Bartlett, Leila Rooshenas, Luke Hughes-Davies, Sarah E Pinder, Peter Hall, Jane Bayani, Jenny L Donovan, Nigel Stallard, David Cameron, Robert Stein, Carrie Cunningham, Adrienne Morgan, Andreas Makris, Monika Sobol, Janet A. Dunn, Christopher McCabe, and Andrea Marshall

Subjects

Oncology, Gerontology, Cancer Research, medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, Cost effectiveness, business.industry, Standard treatment, Population, Cancer, medicine.disease, Clinical trial, Breast cancer, MammaPrint, Internal medicine, medicine, Oncotype DX, business, education

Abstract

Introduction All published adjuvant chemotherapy trials in breast cancer have made the assumption that the proportional benefits of chemotherapy apply uniformly across molecular subgroups. However, it can be argued that chemotherapy effectiveness for luminal A breast cancer is low in comparison to other subtypes irrespective of tumour stage. A logical extension of this argument is that novel multiparametric tests that use biological features of breast cancers to assess risk may also inform chemotherapy benefit in luminal cancers. The OPTIMA trial is a multi-centre, partially blinded, randomised clinical trial with a non-inferiority endpoint, and an adaptive design, to compare standard treatment (chemotherapy followed by endocrine therapy) with multi-parameter test-guided treatment allocation to either chemotherapy followed by endocrine therapy or endocrine therapy alone. OPTIMA-prelim aimed to compare the predicted risk stratification, sub-type classification and cost effectiveness of different multiparameter tests performed on the same patient population. Methods Over 20 months of recruitment 285 patients were randomised to OPTIMA-prelim. Tissue was collected centrally, ER and HER2 status confirmed and samples provided for testing with Oncotype DX™, Prosigna™ (PAM50), Mammaprint™, Mammatyper™, IHC4-AQUA and IHC4 using conventional biomarkers. Sub-type classification was provided by Blueprint™, Mammatyper™ and Prosigna™. Each test was performed at central diagnostic laboratories (OncotypeDx, Mammaprint/Blueprint, Mammatyper) or in a central laboratory (Prosigna™/IHC4) strictly according to GLP practices. Results Samples from 181 patients randomised by January 2014 were tested and data analysed for this study. Patients were categorised as low/intermediate or high risk using predetermined cut-offs for each test. Oncotype DX predicted a proportion of low-risk tumours (79%; 95% CI 73-85%) similar to that predicted as either low or intermediate risk using Prosigna ROR_P (71%; 95% CI 64-78%) and IHC4 (69%; 95% CI 62-76%), whilst MammaPrint identified the fewest low-risk tumours (59%; 95% CI 52-66%). Strikingly, a comparison between tests showed modest agreement between tests when dichotomising results between high vs low/intermediate risk. Disagreement between different tests, in assigning individual tumours to risk categories, is not uncommon; for the four tests [Oncotype DX, MammaPrint, Prosigna ROR_P (low/int) and IHC4 (low/int)], only 71 (39%) tumours were classified as low/intermediate risk for all four tests and only 17 (9%) tumours were high risk for all four tests, 93 (52%) tumours were assigned to different risk categories by different tests. Similarly all three subtypes tests (Blueprint/Prosigna/Mammatyper) each assigned 59% of tumors to luminal A subtype but only 70% of these cases were classified as luminal A by all three assays. Conclusion Existing evidence on the comparative prognostic information provided by different tests suggests current multiparameter tests provide broadly equivalent risk information for the population of women with luminal breast cancers. However, for the individual patient, tests may provide differing risk categorisation or indeed subtype information. Acknowledgement This project was funded by the NIHR Health Technology Assessment (HTA) Programme (project 10/34/01). The opinions expressed therein are those of the authors and do not necessarily reflect those of the HTA programme, NIHR, NHS or Department of Health. Citation Format: John MS Bartlett, Robert C Stein, Jane Bayani, Andrea Marshall, Janet A Dunn, Amy F Campbell, Carrie Cunningham, Monika Sobol, Peter Hall, Leila Rooshenas, Adrienne Morgan, Christopher Poole, Sarah E Pinder, David A Cameron, Nigel Stallard, Jenny Donovan, Christopher McCabe, Luke Hughes-Davies, Andreas Makris, on Behalf of the OPTIMA Trial Management Group. Comparison of multiparameter tests in the UK OPTIMA-Prelim trial [abstract]. In: Proceedings of the Thirty-Seventh Annual CTRC-AACR San Antonio Breast Cancer Symposium: 2014 Dec 9-13; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2015;75(9 Suppl):Abstract nr P4-11-07.

Published

2015

12. Abstract OT3-04-03: PARTNER randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients

Author

A Machin, Jacinta Abraham, H. M. Earl, Ellen Copson, C Harvey, S Thomas, Anne C Armstrong, Luke Hughes-Davies, L Grybowicz, Emma McMurtry, Marc Tischkowitz, Elena Provenzano, Wendi Qian, A-L Vallier, R Roylance, E Chiu, and Karen McAdam

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Anthracycline, business.industry, medicine.medical_treatment, Cancer, medicine.disease, Chemotherapy regimen, Carboplatin, Olaparib, 03 medical and health sciences, Regimen, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Breast cancer, chemistry, 030220 oncology & carcinogenesis, Internal medicine, Medicine, business

Abstract

Background: No specific targeted therapies are available for Triple Negative Breast Cancers (TNBC), an aggressive and diverse subgroup. The basal TNBC subgroup show some phenotypic and molecular similarities with germline BRCA (gBRCA). In gBRCA patients, and potentially other homologous recombination deficiencies, these already compromised pathways may allow drugs called PARP inhibitors (olaparib) to work more effectively. Aims: To establish if the addition of olaparib to neoadjuvant platinum based chemotherapy for basal TNBC and/or gBRCA breast cancer is safe and improves efficacy (pathological complete response (pCR)). Trial design: 3 stage open label randomised phase II/III trial of neoadjuvant paclitaxel and carboplatin +/olaparib, followed by clinicians' choice of anthracycline regimen. Stage 1 and 2: Patients are randomised (1:1:1) to either control (3 weekly carboplatin AUC5/weekly paclitaxel 80mg/m2 for 4 cycles) or one of two research arms with the same chemotherapy regimen but with two different schedules of olaparib 150mg BD for 12 days. Stage 3: Patients are randomised (1:1) to either control arm or to the research arm selected in stage 2. Methods: Stage 1 Safety: both research arms combined. Stage 2 Schedule selection criteria: pCR rate and completion rate of olaparib protocol treatment. It is a “pickthewinner” design with 53 patients in each research arm. This allows a 90% power, 5% onesided significance level to test null hypothesis of pCR ≤35% versus an alternative hypothesis of pCR ≥55% in each of the research arms. Stage 3 Efficacy:anticipated pCR ˜55-60% for all trial patients and ˜60-65% for gBRCA patients. The trial is powered to detect an absolute improvement of 15% (all patients) and 20% (gBRCA patients) by adding olaparib to chemotherapy (enriched design). TNBC patient recruitment will be capped, to ensure required gBRCA patients are enrolled. Enrichment design is applied with overall significance level 0.05(α) = 0.025(αall)+ 0.025(αgBRCA) and 80% power. Target accrual: 527 [gBRCA 220] Current accrual: 56 Sites activated: 15 [expected number of sites 30-50]. Citation Format: Abraham J, Vallier A-L, Qian W, Grybowicz L, Thomas S, Machin A, Harvey C, Chiu E, McAdam K, Hughes-Davies L, Roylance R, Copson E, Armstrong A, Provenzano E, Tischkowitz M, McMurtry E, Earl H. PARTNER randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients [abstract]. In: Proceedings of the 2017 San Antonio Breast Cancer Symposium; 2017 Dec 5-9; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2018;78(4 Suppl):Abstract nr OT3-04-03.

Published

2018

13. Definition of Tumor Bed Boost in Oncoplastic Breast Surgery: An Understanding and Approach

Author

Luke Hughes-Davies, C.E. Coles, E. Garreffa, Amit Agrawal, Sara Lightowlers, and Simon Russell

Subjects

Cancer Research, medicine.medical_specialty, Radiation, Oncology, business.industry, Breast surgery, medicine.medical_treatment, Medicine, Radiology, Nuclear Medicine and imaging, Tumor bed, Radiology, business

Published

2019

14. Abstract OT3-03-03: PARTNER: Randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients

Author

M Weiss, H. M. Earl, Luke Hughes-Davies, Karen McAdam, A Machin, C Harvey, E McMurty, A Roberts, Elena Provenzano, Anne C Armstrong, L Grybowicz, R Roylance, Jacinta Abraham, Ellen Copson, S Thomas, Marc Tischkowitz, K Pinilla, Wendi Qian, and A-L Vallier

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Anthracycline, business.industry, medicine.medical_treatment, Cancer, medicine.disease, Chemotherapy regimen, Carboplatin, Olaparib, chemistry.chemical_compound, Regimen, Breast cancer, chemistry, Internal medicine, medicine, business

Abstract

Background: No specific targeted therapies are available for Triple Negative Breast Cancers (TNBC), an aggressive and diverse subgroup. The basal TNBC sub-group share some phenotypic and molecular similarities with germline BRCA (gBRCA) tumours. In gBRCA patients, and potentially other homologous recombination deficiencies, these already compromised pathways may allow drugs called PARP inhibitors (Olaparib) to work more effectively. Aims: To establish if the addition of olaparib to neoadjuvant platinum based chemotherapy for basal TNBC and/or gBRCA breast cancer is safe and improves efficacy (pathological complete response (pCR)). Methods: Trial design: 3-stage open label randomised phase II/III trial of neoadjuvant paclitaxel and carboplatin +/- olaparib, followed by clinicians' choice of anthracycline regimen. Stage 1 and 2: Randomisation (1:1:1) to either control (3 weekly carboplatin AUC5/weekly paclitaxel 80mg/m2 for 4 cycles) or one of two research arms with the same chemotherapy regimen but with two different schedules of olaparib 150mg BD for 12 days. Stage 3: Patients are randomised (1:1) to either control arm or to the research arm selected in stage 2. End-points: Stage 1: Safety; Stage 2: Schedule selection using pCR rate and completion rate of olaparib using a “pick-the-winner” design. Stage 3: pCR rate. Enrichment design is applied with an overall significance level 0.05(α) and 80% power. A total of 527 patients will be included to detect an absolute improvement of 15% (all patients) and 20% (gBRCA patients) by adding olaparib to platinum based chemotherapy. Trial Progress: PARTNER has been recruiting in UK since 27th May 2016. IDSMC recommended to continue the trial without change after reviewing the Stage 1 safety data. The recruitment of stage 2 was completed in April 2018 and results to be reviewed by the IDSMC in early 2019. The trial is open and enrolling patients to national and international sites. Citation Format: Abraham J, Vallier A-L, Qian W, Machin A, Grybowicz L, Thomas S, Weiss M, Harvey C, McAdam K, Hughes-Davies L, Roberts A, Roylance R, Copson E, Pinilla K, Armstrong A, Provenzano E, Tischkowitz M, McMurty E, Earl H. PARTNER: Randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr OT3-03-03.

Published

2019

15. Abstract OT3-01-02: PARTNERING / PARTNER : Phase II sub-study to establish if the addition of combinations of new agents (olaparib, cell cycle and immune checkpoint inhibitors) can improve the rate of pathological complete response (pCR) and minimal residual disease (MRD) in triple negative breast cancer (TNBC) and / or germline BRCA mutated (gBRCAm) patients with evidence of residual disease after PARTNER therapy

Author

Elena Provenzano, S Thomas, Anne-Laure Vallier, M Weiss, Emma McMurtry, A Machin, Jean Abraham, K Pinilla, Karen McAdam, L Grybowicz, R Roylance, Marc Tischkowitz, Ellen Copson, Anne C Armstrong, C Harvey, Wendi Qian, Luke Hughes-Davies, A Roberts, and H. M. Earl

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Cell cycle checkpoint, business.industry, medicine.medical_treatment, Cancer, medicine.disease, Minimal residual disease, Carboplatin, Olaparib, chemistry.chemical_compound, Breast cancer, chemistry, Internal medicine, Medicine, business, Triple-negative breast cancer, Neoadjuvant therapy

Abstract

Background: In patients with TNBC, following standard neoadjuvant chemotherapy, residual disease (RD) is correlated with poor prognosis and 50% relapse within 5 years [1]. PARTNER is a neoadjuvant clinical trial which randomises TNBC and gBRCAm patients to carboplatin and paclitaxel +/- olaparib followed by anthracycline-based chemotherapy. Patients with RD after neoadjuvant treatment in this trial also face poorer survival outcomes, due to the paucity of treatment options. PARTNERING, develops a new strategy using novel agent combinations as an alternative pathway for patients with RD within the PARTNER trial. Methods: PARTNERING is a phase II open label, sub-study with a two-stage Simon design with biomarker guided treatment cohorts open only to patients in the PARTNER trial. A maximum of 15 patients will be included in each cohort. Patients with RD > 10% tumour cellularity (TC) on biopsy after neoadjuvant therapy will be eligible. Patients who have no tumour cells or < 10% TC, and those with progressive disease will be excluded. Allocation of patients into the cohorts will be based on tumour infiltrating lymphocytes (TILs) expression either on diagnostic or post treatment biopsy. Patients with tumours with TILs score ≤20% are considered “non-immunogenic” They will be stratified according to HRD status and allocated to receive a cell cycle checkpoint inhibitor + olaparib. Patients with a TILs score >20% are considered “immunogenic” and will be allocated to receive an immune checkpoint inhibitor with olaparib or a cell cycle checkpoint inhibitor. Primary outcome measure is pCR / MRD rate at surgery after the administration of 2 cycles / 8 weeks of a combination of new agents. The rate of conversion to pCR/MRD will be correlated with TC, TILs, BRCA and homologous recombination deficiency (HRD) status, Ki67% and previous olaparib treatment. Progress: The PARTNERING pathway in the PARTNER trial will be open late 2018. Citation Format: Abraham JE, Vallier A-L, Qian W, Machin A, Grybowicz L, Thomas S, Weiss M, Harvey C, McAdam K, Hughes-Davies L, Roberts A, Provenzano E, Pinilla K, Roylance R, Copson E, Armstrong A, McMurtry E, Tischkowitz M, Earl HM. PARTNERING / PARTNER : Phase II sub-study to establish if the addition of combinations of new agents (olaparib, cell cycle and immune checkpoint inhibitors) can improve the rate of pathological complete response (pCR) and minimal residual disease (MRD) in triple negative breast cancer (TNBC) and / or germline BRCA mutated (gBRCAm) patients with evidence of residual disease after PARTNER therapy [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr OT3-01-02.

Published

2019

16. PERSEPHONE: 6 versus 12 months (m) of adjuvant trastuzumab in patients (pts) with HER2 positive (+) early breast cancer (EBC): Randomised phase 3 non-inferiority trial with definitive 4-year (yr) disease-free survival (DFS) results

Author

Carlos Caldas, Anne-Laure Vallier, Claire Hulme, Jean Abraham, Louise Hiller, Adrian Harnett, Daniel Rea, Janine Mansi, Helena M. Earl, Andrew M Wardley, Janet A. Dunn, Luke Hughes-Davies, David Miles, Mei-Lin Ah-See, David Cameron, Helen B Higgins, Donna L. Howe, Shrushma Loi, Karen McAdam, and Richard Simcock

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Trastuzumab, 030220 oncology & carcinogenesis, Internal medicine, medicine, Clinical endpoint, Non inferiority trial, In patient, skin and connective tissue diseases, Distributed File System, business, neoplasms, Adjuvant, medicine.drug, Early breast cancer

Abstract

506Background: Adjuvant trastuzumab has significantly improved outcomes for HER2+ EBC pts, using the 12m duration empirically adopted from the pivotal registration trials. A shorter duration could reduce toxicities and cost whilst providing similar efficacy. No reduced-duration trial to date has demonstrated non-inferiority. Methods: PERSEPHONE is a randomised phase 3 non-inferiority trial comparing 6 to 12m trastuzumab, the largest reduced-duration non-inferiority trial internationally. Mapping onto standard UK practice, all HER2+ EBC pts were eligible. Stratification is by ER status, chemotherapy (CT) type, and CT and trastuzumab timing. The primary endpoint is DFS from diagnosis (first relapse or death from any cause). Randomising 4000 pts (1:1) enabled the trial to assess the non-inferiority of 6m (5% 1-sided significance, 85% power), defining non-inferiority as ‘no worse than 3%’ below the 12m arm’s assumed 80% 4-yr DFS. The pre-planned definitive DFS analysis required 500 events. Results: 4089 pts w...

Published

2018

17. Tamoxifen: the drug that came in from the cold

Author

Carlos Caldas, Luke Hughes-Davies, and Gordon C. Wishart

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.drug_class, Estrogen receptor, Breast Neoplasms, breast cancer, Breast cancer, Internal medicine, medicine, Adjuvant therapy, Humans, post-menopausal, skin and connective tissue diseases, Gynecology, Clinical Trials as Topic, Aromatase inhibitor, tamoxifen, Aromatase Inhibitors, business.industry, Estrogen Antagonists, adjuvant therapy, medicine.disease, Antiestrogen, oestrogen receptor, Selective estrogen receptor modulator, Female, Minireview, Breast disease, business, Tamoxifen, medicine.drug

Abstract

Despite the perception of many oncologists that tamoxifen is an inferior drug, and should be substituted by an aromatase inhibitor in post-menopausal women, the current evidence strongly supports the view that AIs should be used 2-3 years after tamoxifen to achieve the maximal overall survival (OS) advantage.

Published

2009

18. Nerve growth factor/nuclear factor-κB pathway as a therapeutic target in breast cancer

Author

Ali Naderi and Luke Hughes-Davies

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Apoptosis, Breast Neoplasms, Receptors, Nerve Growth Factor, chemistry.chemical_compound, Breast cancer, Cell Line, Tumor, Internal medicine, medicine, Humans, Nerve Growth Factors, skin and connective tissue diseases, Receptor, Cell growth, business.industry, NF-kappa B, NF-κB, General Medicine, medicine.disease, Tamoxifen, Nerve growth factor, chemistry, Cell culture, Cancer research, Female, business, Cell Division, medicine.drug

Abstract

Nuclear factor-kappaB pathway (NF-kappaB) is activated in many breast cancers. NF-small kappaB has interactions with other pathways such as the nerve growth factor (NGF) pathway, which is involved in the survival and proliferation of breast cancer cells. NGF treatment of breast cancer cells activates NF-kappaB resulting in the inhibition of ceramide-induced apoptosis. NGF effects on apoptosis and cell proliferation are mediated through p75NTR and p140TrkA receptors, respectively. In this study we investigate the NGF/NF-kappaB pathway as a therapeutic target in breast cancer.We demonstrate that p75NTR inhibitor Pep5, p140TrkA inhibitor K-252a, and NF-kappaB inhibitor BAY11-7085 have pro-apoptotic and anti-proliferation activities in breast cancer cells. We also show a synergy in combining the NGF receptor inhibitors with the conventional breast cancer treatments tamoxifen and taxol.These data suggest that NGF/NF-kappaB pathway is a potential therapeutic target in breast cancer.

Published

2008

19. Efficacy of neoadjuvant bevacizumab added to docetaxel followed by fluorouracil, epirubicin, and cyclophosphamide, for women with HER2-negative early breast cancer (ARTemis) : an open-label, randomised, phase 3 trial

Author

Luke Hughes-Davies, Stephen Chan, David Cameron, Rizvana Ahmad, John M. S. Bartlett, Carlos Caldas, Daniel Rea, Tamas Hickish, Clare Blenkinsop, Jeremy Thomas, Louise Hiller, Ioannis Gounaris, Jean Abraham, Anne-Laure Vallier, Larry Hayward, Helena M. Earl, Stephen Houston, Karen McAdam, L Grybowicz, Janet A. Dunn, and Elena Provenzano

Subjects

Adult, Oncology, medicine.medical_specialty, Bevacizumab, Receptor, ErbB-2, medicine.medical_treatment, Breast Neoplasms, Docetaxel, Antibodies, Monoclonal, Humanized, Disease-Free Survival, Drug Administration Schedule, law.invention, RC0254, Breast cancer, Randomized controlled trial, law, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Clinical endpoint, Humans, Cyclophosphamide, Neoadjuvant therapy, Aged, Epirubicin, business.industry, Middle Aged, medicine.disease, Neoadjuvant Therapy, Fluorouracil, Female, Taxoids, Lymph Nodes, business, medicine.drug

Abstract

Background: The ARTemis trial was developed to assess the efficacy and safety of adding bevacizumab to standard neoadjuvant chemotherapy in HER2-negative early breast cancer.Methods: In this randomised, open-label, phase 3 trial, we enrolled women (≥18 years) with newly diagnosed HER2-negative early invasive breast cancer (radiological tumour size >20 mm, with or without axillary involvement), at 66 centres in the UK. Patients were randomly assigned via a central computerised minimisation procedure to three cycles of docetaxel (100 mg/m2 once every 21 days) followed by three cycles of fluorouracil (500 mg/m2), epirubicin (100 mg/m2), and cyclophosphamide (500 mg/m2) once every 21 days (D-FEC), without or with four cycles of bevacizumab (15 mg/kg) (Bev+D-FEC). The primary endpoint was pathological complete response, defined as the absence of invasive disease in the breast and axillary lymph nodes, analysed by intention to treat. The trial has completed and follow-up is ongoing. This trial is registered with EudraCT (2008-002322-11), ISRCTN (68502941), and ClinicalTrials.gov (NCT01093235).Findings: Between May 7, 2009, and Jan 9, 2013, we randomly allocated 800 participants to D-FEC (n=401) and Bev+D-FEC (n=399). 781 patients were available for the primary endpoint analysis. Significantly more patients in the bevacizumab group achieved a pathological complete response compared with those treated with chemotherapy alone: 87 (22%, 95% CI 18–27) of 388 patients in the Bev+D-FEC group compared with 66 (17%, 13–21) of 393 patients in the D-FEC group (p=0·03). Grade 3 and 4 toxicities were reported at expected levels in both groups, although more patients had grade 4 neutropenia in the Bev+D-FEC group than in the D-FEC group (85 [22%] vs 68 [17%]).Interpretation: Addition of four cycles of bevacizumab to D-FEC in HER2-negative early breast cancer significantly improved pathological complete response. However, whether the improvement in pathological complete response will lead to improved disease-free and overall survival outcomes is unknown and will be reported after longer follow-up. Meta-analysis of available neoadjuvant trials is likely to be the only way to define subgroups of early breast cancer that would have clinically significant long-term benefit from bevacizumab treatment.Funding: Cancer Research UK, Roche, Sanofi-Aventis.

Published

2015

20. Identifying changes in mutational dynamics in patients with early breast cancer undergoing neoadjuvant chemotherapy

Author

S.J. Sammut, Maurizio Callari, H. M. Earl, S.F. Chin, Luke Hughes-Davies, Oscar M. Rueda, Sarah-Jane Dawson, Jean Abraham, Carlos Caldas, and Elena Provenzano

Subjects

Oncology, Cancer Research, Chemotherapy, medicine.medical_specialty, business.industry, medicine.medical_treatment, Internal medicine, medicine, In patient, business, Early breast cancer

Published

2016

21. OPTIMA (Optimal Personalised Treatment of early breast cancer using Multi-parameter Analysis): A prospective trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions

Author

Claire Hulme, Luke Hughes-Davies, Daniel Rea, Andrea Marshall, David Cameron, Iain R. Macpherson, Adele Francis, Leila Rooshenas, Peter Hall, Amy F Campbell, Robert Stein, Victoria Harmer, Andreas Makris, Janet A. Dunn, Helena M. Earl, Sarah E Pinder, Christopher J. Poole, Christopher McCabe, John M. S. Bartlett, and Adrienne Morgan

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Randomization, Axillary lymph nodes, Cost effectiveness, medicine.medical_treatment, Population, law.invention, Breast cancer, Randomized controlled trial, law, Internal medicine, Medicine, Stage (cooking), education, Multi parameter, Early breast cancer, education.field_of_study, Chemotherapy, business.industry, General Medicine, medicine.disease, Surgery, Test (assessment), medicine.anatomical_structure, Prospective trial, business

Abstract

TPS623Background: Multi-parameter gene expression assays (MPAs) are widely used to estimate individual patient residual risk and guide chemotherapy use in hormone sensitive HER2-ve early breast cancer, but prospective validation data are not available. OPTIMA aims to validate the use of MPA testing to predict chemotherapy sensitivity in a largely node-positive breast cancer population. Methods: OPTIMA is a partially blinded multi-center, phase 3 RCT with an adaptive two-stage design. The preliminary phase (OPTIMA prelim) evaluated the performance of MPAs to identify a suitable test to be used in the main efficacy trial, and demonstrated the feasibility and acceptability of a large UK trial. Eligible patients (pts) are men or women aged ≥ 40 years who have surgically resected early stage ER+ve and HER2-ve breast cancer, and have either 1-9 involved axillary lymph nodes or tumors of ≥ 30mm diameter. Randomization is to standard management (chemotherapy followed by endocrine therapy) or to MPA-directed thera...

Published

2016

22. Pneumocystis jiroveci pneumonia (PCP) in patients receiving weekly chemotherapy for metastatic breast cancer

Author

C. Wilson, Carlos Caldas, S.T. Wijaya, Richard D. Baird, M. Moody, Luke Hughes-Davies, Emma Harrison, and Helena M. Earl

Subjects

Weekly chemotherapy, Oncology, medicine.medical_specialty, Pneumonia, business.industry, Internal medicine, medicine, In patient, Hematology, medicine.disease, business, Metastatic breast cancer

Published

2017

23. PARTNER: Randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients

Author

Anne-Laure Vallier, Karen McAdam, Elena Provenzano, Jean Abraham, Helena M. Earl, R Roylance, Ellen Copson, Jessica S. Brown, Wendi Qian, L Grybowicz, Stanly Thomas, Caron Harvey, Luke Hughes-Davies, Saba Mahmud, Emma McMurtry, and Marc Tischkowitz

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Anthracycline, business.industry, medicine.medical_treatment, medicine.disease, Chemotherapy regimen, Carboplatin, Olaparib, 03 medical and health sciences, Regimen, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Breast cancer, chemistry, Paclitaxel, 030220 oncology & carcinogenesis, Internal medicine, Medicine, business

Abstract

TPS591 Background: No specific targeted therapies are available for Triple Negative Breast Cancers (TNBC), an aggressive and diverse subgroup. The basal TNBC sub-group show some phenotypic and molecular similarities with germline BRCA (gBRCA). In gBRCA patients, and potentially other homologous recombination deficiencies, these already compromised pathways may allow drugs called PARP inhibitors (olaparib) to work more effectively. Aims: To establish if the addition of olaparib to neoadjuvant platinum based chemotherapy for basal TNBC and/or gBRCA breast cancer is safe and improves efficacy (pathological complete response (pCR)). Trial design: 3-stage open label randomised phase II/III trial of neoadjuvant paclitaxel and carboplatin +/- olaparib, followed by clinicians' choice of anthracycline regimen. Stage 1 and 2: Patients are randomised (1:1:1) to either control (3 weekly carboplatin AUC5/weekly paclitaxel 80mg/m2 for 4 cycles) or one of two research arms with the same chemotherapy regimen but with two different schedules of olaparib 150mg BD for 12 days. Stage 3: Patients are randomised (1:1) to either control arm or to the research arm selected in stage 2. Methods: Stage 1 - Safety: both research arms combined. Stage 2 - Schedule selection criteria: pCR rate and completion rate of olaparib protocol treatment. It is a “pick-the-winner” design with 53 patients in each research arm. This allows a 90% power, 5% one-sided significance level to test null hypothesis of pCR ≤35% versus an alternative hypothesis of pCR ≥55% in each of the research arms. Stage 3 - Efficacy: anticipated pCR ~55-60% for all trial patients and ~60-65% for gBRCA patients. The trial is powered to detect an absolute improvement of 15% (all patients) and 20% (gBRCA patients) by adding olaparib to chemotherapy (enriched design). TNBC patient recruitment will be capped, to ensure required gBRCA patients are enrolled. Enrichment design is applied with overall significance level 0.05(α) = 0.025(αall)+ 0.025(αgBRCA) and 80% power. Target accrual: 527 [gBRCA 220] Current accrual: 17 Sites activated: 12 [expected number of sites 30-50].

Published

2017

24. Abstract OT2-01-15: PARTNER - Randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients

Author

Ellen Copson, Luke Hughes-Davies, S Mahmud, Karen McAdam, R Roylance, J Brown, Jean Abraham, Marc Tischkowitz, Wendi Qian, Elena Provenzano, S Thomas, L Grybowicz, A-L Vallier, C Harvey, and H. M. Earl

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Performance status, business.industry, Standard treatment, Cancer, medicine.disease, Chemotherapy regimen, Carboplatin, Olaparib, 03 medical and health sciences, Regimen, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Breast cancer, chemistry, 030220 oncology & carcinogenesis, Internal medicine, medicine, business

Abstract

Background: Triple Negative Breast Cancers (TNBC) are a biologically diverse and aggressive sub-group. Early effective treatment can lead to cure. Current standard treatment is systemic chemotherapy either pre-/post-definitive surgery. No specific targeted therapies are available for TNBC. There are phenotypic and molecular similarities between germline BRCA (gBRCA) breast cancer and TNBC. In TNBC 10%-20% harbour gBRCA mutations. In gBRCA patients, and potentially other homologous recombination deficiencies, these already compromised pathways allow drugs called PARP inhibitors (olaparib) to work particularly effectively. Aims: To establish if the addition of olaparib to neoadjuvant platinum-based chemotherapy for TNBC and/or gBRCA breast cancer is safe and improves efficacy. Trial design: 3-stage open label randomised phase II/III trial of neoadjuvant olaparib +/- platinum containing chemotherapy followed by clinicians' choice of anthracycline regimen. Stage 1 and 2, patients are randomised (1:1:1) to either control (3 weekly carboplatin AUC5/weekly paclitaxel 80mg/m2 chemotherapy - 4 cycles) or one of two research arms which uses the same chemotherapy regimen but with two different schedules of olaparib 150mg BD). Stage 3: patients are randomised (1:1) to either control arm or to the research arm selected in stage 2. Primary outcome measures: Stage 1: safety of the addition of olaparib to chemotherapy. Prophylactic G-CSF is mandatory. Stage 2: pathological complete response (pCR) in each of the two research arms. At the end of stage 2, one of the research arms will be dropped. Stage 3: pCR at surgery after neoadjuvant treatment. pCR - defined as no residual invasive carcinoma within the breast (ductal carcinoma in situ permitted) AND no evidence of metastatic disease within the lymph nodes. Eligibility: •Aged 16 to 70. •Written informed consent. •Histologically confirmed invasive breast cancer. •Clinical stage T1-4 N0-2 (tumour or metastatic node diameter>10mm) •Confirmed ER-negative and HER2-negative or gBRCA mutation positive, irrespective of hormone status. •Performance Status 0-1 Statistical Methods: Stage 1, Safety: both research arms combined. Stage 2, Schedule selection criteria: pCR rate and completion rate of olaparib protocol treatment. It is a “pick-the winner” design with 53 patients in each research arm. This allows a 90% power, 5% one-sided significance level to test null hypothesis of pCR ≤35% versus an alternative hypothesis of pCR ≥55% in each of the research arms. Stage 3, Efficacy: anticipated pCR ∼45-55% for all trial patients and ∼50-60% for gBRCA patients. The trial is powered to detect an absolute improvement of 15% (all patients) and 20% (gBRCA patients) by adding olaparib to chemotherapy (enriched design). TNBC patient recruitment will be capped, to ensure the required number of gBRCA patients are enrolled. Enrichment design is applied with the overall significance level 0.05(α)=0.025(αall)+ 0.025(αgBRCA) and 80% power. Present accrual: 1 [Trial opened: 23rd May 2016] Target accrual: 527 (TNBC 307; gBRCA 220) Contact information: Dr. Jean Abraham; Email: ja344@medschl.cam.ac.uk. Citation Format: Abraham JE, Vallier A-L, Qian W, Grybowicz L, Thomas S, Mahmud S, Harvey C, McAdam K, Hughes-Davies L, Roylance R, Copson E, Brown J, Provenzano E, Tischkowitz M, Earl HM. PARTNER - Randomised, phase II/III trial to evaluate the safety and efficacy of the addition of olaparib to platinum-based neoadjuvant chemotherapy in triple negative and/or germline BRCA mutated breast cancer patients [abstract]. In: Proceedings of the 2016 San Antonio Breast Cancer Symposium; 2016 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2017;77(4 Suppl):Abstract nr OT2-01-15.

Published

2017

25. Barriers to protocol-led early discharge of low-risk febrile neutropenia patients

Author

S. Kim, E. Day, and Luke Hughes-Davies

Subjects

Patient discharge, Risk, Pediatrics, medicine.medical_specialty, business.industry, MEDLINE, medicine.disease, Patient Discharge, Oncology, medicine, Humans, Radiology, Nuclear Medicine and imaging, business, Early discharge, Febrile neutropenia, Febrile Neutropenia

Published

2014

26. Abstract PD2-3: ARTemis: A randomised trial of bevacizumab with neo-adjuvant chemotherapy for patients with HER2-negative early breast cancer

Author

Luke Hughes-Davies, Stephen Chan, Louise Hiller, Tamas Hickish, Jeremy Thomas, Rizvana Ahmad, David Cameron, Jean Abraham, Helena M. Earl, Clare Blenkinsop, Larry Hayward, Daniel Rea, Elena Provenzano, John M. S. Bartlett, Janet A. Dunn, Anne-Laure Vallier, Stephen Houston, L Grybowicz, Carlos Caldas, and Karen McAdam

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, business.industry, HER2 negative, Surgery, Internal medicine, medicine, business, Neo adjuvant chemotherapy, Early breast cancer, medicine.drug

Abstract

Background: Bevacizumab (bev) has been used with neo-adjuvant chemotherapy (NACT) in breast cancer trials. Geparquinto reported benefit for bev in triple negative (neg) patients (pts) (pathological complete response (pCR) 36.4% vs 27.8% p=0.02), as did CALGB 40603 (pCR 52% vs 44%, p=0.057), although NSABP-B40 showed benefit in ER positive (pos) pts (pCR 23.3% vs 15.2%, p=0.008). Methods: ARTemis is a randomised phase 3 trial adding bev to NACT (docetaxel (D)-FEC). Pts with HER2-neg invasive breast cancer were eligible. Stratification was by age, ER status (neg:weak pos:strong pos), tumour size (T2:T3/4), clinical involvement of axillary nodes and inflammatory/locally advanced disease. Pts were randomised (1:1) to bev+D-FEC or D-FEC. The primary endpoint was pCR, defined as no residual invasive cancer in the breast or axillary lymph nodes after NACT. 800 pts were required to detect 10% differences in pCR rates; 85% power, 5% alpha level. Results: 800 pts were randomised from 66 UK centres (May 2009 to Jan 2013). 68% were D→FECBev+D→FEC % (95%CI)% (95%CI)p *$pCR in all breast tumours AND absence of disease in ax LNs in all breast tumours(n=66/393)(n=87/388) 17% (13-21%)22% (18-27%)0.03 ER neg (Allred 0-2) (n=253)32% (24-41)44% (36-54) ER weak pos (Allred 3-5) (n=67)26% (13-44)52% (34-69) ER strong pos (Allred 6-8) (n=461)7% (4-11)6% (3-10) pCR or MRD in all breast tumours(n=114/394)(n=138/388) 29% (25-34%)36% (31-41%)0.035 ER neg (Allred 0-2) (n=254)45% (36-54)56% (47-65) ER weak pos (Allred 3-5) (n=67)44% (27-62)73% (54-87) ER strong pos (Allred 6-8) (n=461)18% (13-23)19% (14-24) * Adjusted for stratification variables. $ Primary endpoint for the ARTemis trial Conclusions: ARTemis showed a significant improvement in both pCR and MRD rates with the addition of bev to D-FEC. ER-neg and ER-weak pos / HER2-neg breast cancer pts appeared to benefit most from bev, whilst pCR and MRD rates in ER-strong pos pts were lower and did not appear to benefit from bev. Our results are similar to those reported in Geparquinto and CALGB 40603. Citation Format: Helena M Earl, Louise Hiller, Janet A Dunn, Clare Blenkinsop, Louise Grybowicz, Anne-Laure Vallier, Jean Abraham, Jeremy Thomas, Elena Provenzano, Luke Hughes-Davies, Karen McAdam, Stephen Chan, Rizvana Ahmad, Tamas Hickish, Stephen Houston, Daniel Rea, John Bartlett, Carlos Caldas, David Cameron, Larry Hayward. ARTemis: A randomised trial of bevacizumab with neo-adjuvant chemotherapy for patients with HER2-negative early breast cancer [abstract]. In: Proceedings of the Thirty-Seventh Annual CTRC-AACR San Antonio Breast Cancer Symposium: 2014 Dec 9-13; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2015;75(9 Suppl):Abstract nr PD2-3.

Published

2015

27. OPTIMA: a prospective randomised trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions

Author

Iain R. Macpherson, Janet A. Dunn, Carmel Conefrey, Christopher McCabe, Daniel Rea, Adele Francis, Robert Stein, Peter Hall, Victoria Harmer, John M. S. Bartlett, Helena M. Earl, Andrea Marshall, Sarah E Pinder, Helen B Higgins, Amy F Campbell, Leila Rooshenas, Christopher J. Poole, Claire Hulme, Andreas Makris, Adrienne Morgan, Jenny L Donovan, Luke Hughes-Davies, and David Cameron

Subjects

Oncology, medicine.medical_specialty, Chemotherapy, business.industry, Cost effectiveness, 030503 health policy & services, medicine.medical_treatment, General Medicine, Test (assessment), 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Physical therapy, Medicine, Surgery, 030212 general & internal medicine, 0305 other medical science, business

Published

2016

28. Disease-free (DFS) and overall survival (OS) at 3.4 years (yrs) for neoadjuvant bevacizumab (Bev) added to docetaxel followed by fluorouracil, epirubicin and cyclophosphamide (D-FEC), for women with HER2 negative early breast cancer: The ARTemis trial

Author

Anne-Laure Vallier, L Grybowicz, Rizvana Ahmad, Tamas Hickish, Jeremy Thomas, Carlos Caldas, Janet A. Dunn, John M. S. Bartlett, Daniel Rea, Elena Provenzano, Stephen Houston, Karen McAdam, Luke Hughes-Davies, Clare Blenkinsop, David Cameron, Jean Abraham, Helena M. Earl, Larry Hayward, Louise Hiller, and Stephen Chan

Subjects

Gynecology, Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, Cyclophosphamide, business.industry, 030503 health policy & services, HER2 negative, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Docetaxel, Fluorouracil, 030220 oncology & carcinogenesis, Internal medicine, medicine, skin and connective tissue diseases, 0305 other medical science, business, medicine.drug, Epirubicin, Early breast cancer

Abstract

1014Background: ARTemis compared the addition of Bev to neoadjuvant D-FEC in HER2 negative breast cancer. Improved pathological complete response (pCR) with Bev has been reported previously. Method...

Published

2016

29. Comparing Breast Cancer Multiparameter Tests in the OPTIMA Prelim Trial: No Test Is More Equal Than the Others

Author

Andrea Marshall, Peter Hall, Daniel Rea, John M. S. Bartlett, Monika Sobol, Iain R. Macpherson, Jane Bayani, Peter Canney, Andreas Makris, Christopher J. Poole, Robert Stein, Christopher McCabe, Helena M. Earl, Sarah E Pinder, Janet A. Dunn, Amy F Campbell, Carrie Cunningham, Adele Francis, Luke Hughes-Davies, and David Cameron

Subjects

Adult, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Antineoplastic Agents, Hormonal, Receptor, ErbB-2, Clinical Decision-Making, Population, Breast Neoplasms, Risk Assessment, Decision Support Techniques, RC0254, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, MammaPrint, Predictive Value of Tests, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Confidence Intervals, medicine, Humans, PAM50 Gene Expression Signature, education, Aged, Gynecology, education.field_of_study, medicine.diagnostic_test, Oncotype DX Breast Cancer Assay, business.industry, Middle Aged, Nomogram, Prognosis, medicine.disease, Tumor Burden, Nomograms, 030104 developmental biology, Receptors, Estrogen, Lymphatic Metastasis, 030220 oncology & carcinogenesis, Predictive value of tests, Female, Neoplasm Recurrence, Local, Oncotype DX, business

Abstract

Background: Previous reports identifying discordance between multiparameter tests at the individual patient level have been largely attributed to methodological shortcomings of multiple in silico studies. Comparisons between tests, when performed using actual diagnostic assays, have been predicted to demonstrate high degrees of concordance. OPTIMA prelim compared predicted risk stratification and subtype classification of different multiparameter tests performed directly on the same population.\ud \ud Methods: Three hundred thirteen women with early breast cancer were randomized to standard (chemotherapy and endocrine therapy) or test-directed (chemotherapy if Oncotype DX recurrence score >25) treatment. Risk stratification was also determined with Prosigna (PAM50), MammaPrint, MammaTyper, NexCourse Breast (IHC4-AQUA), and conventional IHC4 (IHC4). Subtype classification was provided by Blueprint, MammaTyper, and Prosigna.\ud \ud Results: Oncotype DX predicted a higher proportion of tumors as low risk (82.1%, 95% confidence interval [CI] = 77.8% to 86.4%) than were predicted low/intermediate risk using Prosigna (65.5%, 95% CI = 60.1% to 70.9%), IHC4 (72.0%, 95% CI = 66.5% to 77.5%), MammaPrint (61.4%, 95% CI = 55.9% to 66.9%), or NexCourse Breast (61.6%, 95% CI = 55.8% to 67.4%). Strikingly, the five tests showed only modest agreement when dichotomizing results between high vs low/intermediate risk. Only 119 (39.4%) tumors were classified uniformly as either low/intermediate risk or high risk, and 183 (60.6%) were assigned to different risk categories by different tests, although 94 (31.1%) showed agreement between four of five tests. All three subtype tests assigned 59.5% to 62.4% of tumors to luminal A subtype, but only 121 (40.1%) were classified as luminal A by all three tests and only 58 (19.2%) were uniformly assigned as nonluminal A. Discordant subtyping was observed in 123 (40.7%) tumors.\ud \ud Conclusions: Existing evidence on the comparative prognostic information provided by different tests suggests that current multiparameter tests provide broadly equivalent risk information for the population of women with estrogen receptor (ER)–positive breast cancers. However, for the individual patient, tests may provide differing risk categorization and subtype information.

Published

2016

30. Abstract OT3-02-12: OPTIMA (optimal personalised treatment of early breast cancer usIng multi-parameter analysis), a prospective trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions

Author

Robert Stein, Janet A. Dunn, Christopher McCabe, Leila Rooshenas, Claire Hulme, Anna Campbell, Victoria Harmer, Adele Francis, Christopher J. Poole, Nigel Stallard, Adrienne Morgan, Andreas Makris, Andrea Marshall, D.W. Rea, Jms Bartlett, Sarah E Pinder, Jenny L Donovan, Luke Hughes-Davies, Peter Hall, David Cameron, H. M. Earl, and Iain R. Macpherson

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, Randomization, medicine.diagnostic_test, Cost effectiveness, business.industry, Population, Cancer, medicine.disease, law.invention, Breast cancer, Quality of life, Randomized controlled trial, law, Internal medicine, medicine, Oncotype DX, education, business

Abstract

Background: Multi-parameter gene expression assays (MPAs) are widely used to estimate individual patient residual risk and to guide chemotherapy use in hormone-sensitive HER2-negative node-negative early breast cancer. These uses of MPAs have not yet been prospectively validated. OPTIMA aims to validate the use of MPA testing to predict chemotherapy sensitivity in a largely node-positive breast cancer population. Methods: OPTIMA is a partially blinded multi-center, phase 3 randomized controlled trial with an adaptive two-stage design. The preliminary phase (OPTIMA prelim) evaluated the performance of MPAs to identify a suitable test(s) to be used in the main efficacy trial and assessed the feasibility and acceptability of a large UK trial. Eligible patients are men or women aged 40 years or older who have surgically resected early stage breast cancer, which is ER-positive and HER2-negative and who have either 1-9 involved axillary lymph nodes or tumors of at least 30mm diameter. Randomization is to standard management (chemotherapy followed by endocrine therapy) or to MPA-directed treatment. Those with a tumor categorized as "high-risk" by the test will be assigned to standard management whilst those at "low-risk" will be treated with endocrine therapy alone. OPTIMA prelim used Oncotype DX as the primary discriminator; the main trial will use Prosigna (PAM50). The co-primary outcomes are (1) Invasive Disease Free Survival (IDFS) and (2) cost-effectiveness of test-directed therapy compared to standard practice. Secondary outcomes include IDFS in "low-risk" patients, distant disease free survival, breast cancer specific survival, overall survival and quality of life. An integrated qualitative recruitment study will identify and address challenges to recruitment and informed consent. Tumor blocks from all consenting participants will be banked allowing the performance of alternative MPA technologies to be evaluated. Recruitment of 4500 patients over 4 years will permit demonstration of 3% non-inferiority of test-directed treatment, with 5% significance and 85% power, assuming 3 years follow-up and a control arm 5-year IDFS of at least 85%. The addition of patients from OPTIMA prelim will allow non-inferiority to be assessed with 2.5% significance. Results: OPTIMA-prelim recruited 412 patients in 23 months from 35 sites. It confirmed the acceptability of randomization to patients with a 47% acceptance rate, and to clinicians and hence the feasibility of a large prospective trial of test-directed treatment running in 100-plus UK sites. It showed that investment into research on test-directed therapy, especially with Prosigna, should be of substantial value to the NHS. Conclusion: OPTIMA, as one of two large scale prospective trials validating the use of test-guided chemotherapy in node-positive hormone-sensitive early breast cancer will have a global impact on patient treatment. Recruitment into the main efficacy trial will commence in October 2015. Funding: Project funded by the UK NIHR HTA Programme (10/34/501). Views expressed are those of the authors and not those of the HTA Programme, NIHR, NHS or the DoH. Citation Format: Stein RC, Marshall A, Hall PS, Bartlett JMS, Rooshenas L, Campbell A, Cameron DA, Rea D, Macpherson I, Earl HM, Poole CJ, Francis A, Morgan A, Harmer V, Pinder SE, Stallard N, Donovan J, Hulme C, McCabe C, Hughes-Davies L, Makris A, Dunn JA. OPTIMA (optimal personalised treatment of early breast cancer usIng multi-parameter analysis), a prospective trial to validate the predictive utility and cost-effectiveness of gene expression test-directed chemotherapy decisions. [abstract]. In: Proceedings of the Thirty-Eighth Annual CTRC-AACR San Antonio Breast Cancer Symposium: 2015 Dec 8-12; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2016;76(4 Suppl):Abstract nr OT3-02-12.

Published

2016

31. Selecting breast cancer patients for chemotherapy: the opening of the UK OPTIMA trial

Author

Adrienne Morgan, A. M. Campbell, Luke Hughes-Davies, David Cameron, Claire Hulme, Helena M. Earl, Daniel Rea, Christopher McCabe, Sarah E Pinder, Jenny L Donovan, Peter Canney, Peter Hall, Jms Bartlett, Christopher J. Poole, L. Hillier, Nigel Stallard, Helen B Higgins, Janet A. Dunn, V. Harmer, Adele Francis, Robert Stein, and Andreas Makris

Subjects

Gynecology, medicine.medical_specialty, Chemotherapy, business.industry, Tumor biology, medicine.medical_treatment, Patient Selection, MEDLINE, Endocrine therapy, Breast Neoplasms, Intensive chemotherapy, medicine.disease, United Kingdom, Breast cancer, Oncology, Chemotherapy, Adjuvant, medicine, Humans, Radiology, Nuclear Medicine and imaging, Female, Relapse risk, Intensive care medicine, business, Adjuvant, Randomized Controlled Trials as Topic

Abstract

The mortality from breast cancer has improved steadily over the past two decades, in part because of the increased use of more effective adjuvant therapies. Thousands of women are routinely treated with intensive chemotherapy, which can be unpleasant, is expensive and is occasionally hazardous. Oncologists have long known that some of these women may not need treatment, either because they have a low risk of relapse or because they have tumour biology that makes them less sensitive to chemotherapy and more suitable for early adjuvant endocrine therapy. There is an urgent need to improve patient selection so that chemotherapy is restricted to those patients who will benefit from it. Here we review the emerging technologies that are available for improving patient selection for chemotherapy. We describe the OPTIMA trial, which has just opened to recruitment in the UK, is the latest addition to trials in this area, and is the first to focus on the relative cost-effectiveness of alternate predictive assays.

Published

2012

32. Training the oncologists of the future

Author

J. Barrett and Luke Hughes-Davies

Subjects

Male, Medical education, business.industry, Medical school, Medical Oncology, Training (civil), United Kingdom, Oncology, Physicians, Workforce, Medicine, Humans, Radiology, Nuclear Medicine and imaging, Female, business, Forecasting

Abstract

This pair of editorials considers the early years of training. These years begin at medical school, where students are exposed to a large number of specialties, each ofwhich has to compete for talent. Specialities that have helicopters landing on the hospital roof have an obvious initial advantage, but the best recruitment tool is excellent teaching; if we can deliver this, we will attract the best students. First, Luke HughesDavies discusses medical school teaching and then Jane Barrett considers the next step: recruitment into our training programmes.

Published

2011

33. The International Core Literature Consensus (ICLC): an alternative curriculum for Oncologists

Author

Reshma Jagsi, Natalie Cook, Shilpen Patel, Luke Hughes-Davies, and Christine Parkinson

Subjects

medicine.medical_specialty, Consensus, education, Pharmacology toxicology, Alternative medicine, MEDLINE, Breast Neoplasms, Medical Oncology, Nursing, Education, Professional, Medicine, Humans, Curriculum, Medical education, Radiotherapy, business.industry, Public Health, Environmental and Occupational Health, International Agencies, Core (game theory), Oncology, Radiation Oncology, Female, Clinical Competence, Clinical competence, business

Abstract

Oncologists must familiarize themselves with a complex evidence base. Several curricula have been devised, but it is not clear how these are used. We chose breast cancer, since this has a large literature base. Of the 285 radiation and medical oncology trainees in the USA and UK responding to our survey, over 90% reported knowledge of the literature was essential. Just over half of respondents had actually read the ASCO or ESMO curricula, with only 23% reporting that the curricula were important in their learning. Our survey revealed dissatisfaction with current curricula and a demand for more pragmatic literature guidance. We designed an alternative curriculum by using a 21-member peer review group to validate a list of key papers in breast oncology. Oncologists in training need guidance to direct their study. A curriculum based on an International Core Literature Consensus might match the needs of trainees more closely.

Published

2011

34. Practicalities of using an adaptive design for decision making within the optima trial: optimal personalized treatment of early breast cancer using multi-parameter tests

Author

Daniel Rea, Luke Hughes-Davies, David Cameron, Helena M. Earl, Iain R. Macpherson, Adele Francis, Nigel Stallard, Janet A. Dunn, Amy F Campbell, Robert Stein, Andreas Makris, Victoria Harmer, Andrea Marshall, Adrienne Morgan, and Christopher J. Poole

Subjects

Oncology, medicine.medical_specialty, education.field_of_study, business.industry, Personalized treatment, Population, Medicine (miscellaneous), medicine.disease, Bioinformatics, Breast cancer, Internal medicine, Adaptive design, Poster Presentation, medicine, Pharmacology (medical), business, education, Multi parameter, Selection (genetic algorithm), Early breast cancer

Abstract

Multi-parameter gene expression assays (MPA) to aid selection of chemotherapy in hormone-sensitive early breast cancer have not been prospectively validated. This field of personalised medicine is rapidly evolving. There is currently no “best test”. OPTIMA is an adaptive trial of MPA-based chemotherapy assignment in a largely node-positive breast cancer population.

Published

2015

35. 1809 Results of the OPTIMA (Optimal Personalized Treatment of early breast cancer usIng Multi-parameter Analysis) prelim study

Author

Iain R. Macpherson, Claire Hulme, H. M. Earl, Andreas Makris, Jms Bartlett, Christopher McCabe, Robert Stein, Adrienne Morgan, Christopher J. Poole, Luke Hughes-Davies, Adele Francis, David Cameron, Nigel Stallard, Janet A. Dunn, Andrea Marshall, Anna Campbell, Peter Hall, D.W. Rea, Peter Canney, and Sarah E Pinder

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Internal medicine, Personalized treatment, medicine, business, Multi parameter, Early breast cancer

Published

2015

36. Amplification of the BRCA2 pathway gene EMSY in sporadic breast cancer is related to negative outcome

Author

Charles Theillet, Hélène Vallès, Lisa Ursule, Luke Hughes-Davies, Marguerite Cuny, Béatrice Orsetti, Tony Kouzarides, and Carmen Rodríguez

Subjects

Cancer Research, Candidate gene, Tumor suppressor gene, Centromere, Locus (genetics), Breast Neoplasms, Biology, Cohort Studies, Gene duplication, Tumor Cells, Cultured, Humans, Neoplasm Invasiveness, Gene, Retrospective Studies, BRCA2 Protein, Chromosomes, Human, Pair 11, Carcinoma, Ductal, Breast, Gene Amplification, Chromosome, Nuclear Proteins, Amplicon, Prognosis, Molecular biology, Neoplasm Proteins, Repressor Proteins, Carcinoma, Lobular, Real-time polymerase chain reaction, Oncology, Cancer research, Female, Signal Transduction

Abstract

DNA amplification at band q13 of chromosome 11 is common in breast cancer, and CCND1 and EMS1 remain the strongest candidate genes. However, amplification patterns are consistent with the existence of four cores of amplification, suggesting the involvement of additional genes. Here we present evidence strongly suggesting the involvement of the recently characterized EMSY gene in the formation of the telomeric amplicon. EMSY maps at 11q13.5, 100 kb centromeric to the GARP gene, which has been mapped within the core of the distal amplicon. The EMSY protein was shown to interact with BRCA2 and has a role in chromatin remodeling. This makes EMSY a strong candidate oncogene for the 11q13.5 amplicon. DNA amplification was studied in a total of 940 primary breast tumors and 39 breast cancer cell lines. Amplification profiles were consistent with the EMSY-GARP locus being amplified independently of CCND1 and/or EMS1. EMSY RNA expression levels were studied along with those of five other genes located at 11q13.5 by real-time quantitative PCR in the 39 cell lines and a subset of 65 tumors. EMSY overexpression correlated strongly with DNA amplification in both primary tumors and cell lines. In a subset of 296 patients, EMSY amplification was found by both uni- and multivariate analyses to correlate with shortened disease-free survival. These data indicate that EMSY is a strong candidate oncogene for the 11q13.5 amplicon.

Published

2004

37. ARTemis: A randomised trial of bevacizumab with neoadjuvant chemotherapy (NACT) for patients with HER2-negative early breast cancer—Primary endpoint, pathological complete response (pCR)

Author

Richard L Hayward, Tamas Hickish, Jeremy Thomas, John M. S. Bartlett, Rizvana Ahmad, Karen McAdam, Clare Blenkinsop, Daniel Rea, Louise Hiller, Elena Provenzano, Anne-Laure Vallier, Jean Abraham, Steve Chan, L Grybowicz, Carlos Caldas, Helena M. Earl, Stephen Houston, Janet A. Dunn, Luke Hughes-Davies, and David Cameron

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Bevacizumab, business.industry, medicine.medical_treatment, HER2 negative, medicine.disease, Surgery, Breast cancer, Internal medicine, medicine, Clinical endpoint, skin and connective tissue diseases, business, Pathological, Complete response, medicine.drug, Early breast cancer

Abstract

1014 Background: Bevacizumab (bev) has been used with NACT in breast cancer trials. Geparquinto reported benefit for bev in triple negative (neg) patients (pts) (pCR 36.4% v 27.8% p=0.02), as did C...

Published

2014

38. Stage IA-IIB Hodgkin's disease: management and outcome of extensive thoracic involvement

Author

Rita M. Linggood, Luke Hughes-Davies, Peter Mauch, C. Norman Coleman, George P. Canellos, Nancy J. Tarbell, Barbara Silver, and Lawrence N. Shulman

Subjects

Cancer Research, medicine.medical_specialty, medicine.medical_treatment, Mediastinal Neoplasms, Disease-Free Survival, Laparotomy, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Radiology, Nuclear Medicine and imaging, Myocardial infarction, Treatment Failure, Stage (cooking), Pneumonitis, Neoplasm Staging, Radiation, medicine.diagnostic_test, business.industry, Mediastinum, Combination chemotherapy, medicine.disease, Combined Modality Therapy, Hodgkin Disease, Surgery, Radiation therapy, Radiation Pneumonitis, Survival Rate, medicine.anatomical_structure, Oncology, business, Chest radiograph

Abstract

Purpose: To examine the presentation, management, and outcome of patients with extensive intrathoracic involvement in early-stage Hodgkin's disease. Patients and Methods: One hundred seventy-two patients with clinical Stage IA-IIB Hodgkin's disease and extensive intrathoracic involvement were studied. Extensive intrathoracic disease was defined as either large mediastinal adenopathy (LMA, defined as the width of the mass greater than one-third the maximum thoracic diameter, n = 154) or as extensive (>10 cm) cephalocaudad intrathoracic disease that did not fulfill formal chest radiograph criteria for LMA (n = 18). Patients were divided into three groups based on staging and extent of treatment. Forty-seven patients were treated with radiation alone after a laparotomy (RT-lap), 47 patients received combined modality therapy after laparotomy (CMT-lap), and 78 patients were treated with combined modality therapy without staging laparotomy ( CMT-no lap). MOPP was used in 82% of the CMT patients. Low-dose whole-cardiac RT was used in nearly 50% of patients treated either with RT or CMT. Results: The 10-year actuarial freedom from relapse rates were 54% with RT alone and 88% with CMT (p = 0.001); overall survival rates were 84 and 89%, respectively (p = NS). The median time to relapse was only 17 months. Over 80% of relapses occurred within the first 3 years. The most common site of relapse in all patients was the mediastinum. Relapses below the diaphragm were rare, even in CMT patients who did not receive abdominal radiation treatment. The principal acute morbidity was symptomatic pneumonitis, which occurred in 29% of patients receiving any part of their chemotherapy after RT, compared to 13% if all the chemotherapy was given before RT and 11% if RT alone was administered. There was a low late risk of myocardial infarction (3%) in the two groups with the longest follow up (RT-lap, CMT-lap), but a higher risk of second malignancy in the CMT-lap group (21%) compared with the RT-lap group (2%). Conclusion: Extensive intrathoracic involvement is a distinctive presentation of early-stage HD that has a high relapse risk if treated with RT alone. The introduction of CMT has been associated with improvements in freedom from relapse. The low rate of peripheral relapse with CMT suggests that reductions in field size may be achievable. The use of low-dose whole-heart RT with modern techniques is not associated with a high risk of late cardiac complications and should be used in patients who present with extensive pericardial disease or cardiophrenic lymphadenopathy. The high rate of second malignancy in the CMT group with the longest follow-up suggests that careful long-term surveillance for such patients is warranted.

Published

1997

39. OPTIMA prelim: Optimal personalized treatment of early breast cancer using multiparameter tests

Author

Adrienne Morgan, Amy F Campbell, Andrea Marshall, Peter Hall, Helen B Higgins, Victoria Harmer, Luke Hughes-Davies, Peter Canney, Janet A. Dunn, Jenny L Donovan, Daniel Rea, Christopher McCabe, Claire Hulme, David Cameron, Andreas Makris, Sarah E Pinder, Adele Francis, Nigel Stallard, John M. S. Bartlett, and Robert Stein

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Pathology, Chemotherapy, business.industry, medicine.medical_treatment, Personalized treatment, Internal medicine, HER2 Gene Amplification, medicine, business, Early breast cancer

Abstract

TPS656 Background: Chemotherapy may have little effect on some subtypes of early breast cancer, identified as being hormonally responsive tumours without HER2 gene amplification and with a low or intermediate grade. Multi-parameter genomic tests such as Oncotype DX are increasingly used to identify patients for whom the addition of chemotherapy may confer little additional benefit. OPTIMA has an adaptive design seeking to advance development of personalised medicine in breast cancer by assessing the value of multi-parameter tests in a UK population of intermediate risk. Methods: OPTIMA prelim, the feasibility phase, has 3 objectives: (1) To evaluate performance and health-economics of multi-parameter tests to determine which test(s) will be used in the main trial; (2) To establish efficient and timely sample collection and analysis essential to deliver multi-parameter test driven treatment; (3) To establish the acceptability to patients and clinicians of randomisation to test-directed treatment assignment. OPTIMA prelim aims to recruit 300 patients with ER+ve HER2-ve tumours with involved nodes (pN1-2). Patients are randomized to the standard arm of chemotherapy with endocrine therapy, or to the “test-directed treatment” arm assigned to either the same chemotherapy with endocrine therapy or endocrine therapy only according to the result of an Oncotype DX test. The decision to continue to a main trial will be determined by concordance, cost and willingness of patients to be randomized to test guided treatment. Cost-effectiveness models will be based on the model developed in preparation for the OPTIMA trial, updated with contemporary evidence from the feasibility study and appropriate external data, e.g. the Ontario prospective cohort study. Results: Optima opened in Sept 2012 with 25 centres involved. To date 22 patients are registered, of which 17 have been randomised. Patient focus groups show the trial design is acceptable and has potential to reduce need for chemotherapy. TSC and DMEC agree that this is an important trial testing the feasibility within this patient population. Decision rules are challenging for this study but employment of adaptive designs gives the flexibility needed for the main trial. Clinical trial information: ISRCTN42400492.

Published

2013

40. Neo-tAnGo science: A translational study of PAM 50 sub-typing in sequential fresh tissue samples during neoadjuvant chemotherapy

Author

Roslin Russell, Carlos Caldas, Mark J Dunning, Luke Hughes-Davies, Elena Provenzano, Oscar M. Rueda, Linda Jones, Christopher J. Gallagher, Diana Ritchie, Steve Chan, Janet A. Dunn, Anthony Skene, Suet-Feung Chin, Nicholas P. Murray, A-L Vallier, Kim Benstead, Louise Hiller, Helena M. Earl, Mahesh Iddawela, and Jean Abraham

Subjects

Gynecology, Cancer Research, Chemotherapy, medicine.medical_specialty, Anthracycline, business.industry, medicine.medical_treatment, medicine.disease, Minimal residual disease, Gastroenterology, Gemcitabine, Basal (phylogenetics), Breast cancer, Oncology, Fresh Tissue, Internal medicine, Medicine, Sub typing, business, medicine.drug

Abstract

1015 Background: Neo-tAnGo was an NCRI UK neoadjuvant breast cancer study testing the addition of gemcitabine to anthracycline and taxane-based treatment and also the sequencing of chemotherapy. In a translational substudy, sequential fresh tissue was analysed for PAM 50 subgroups. Methods: Neo-tAnGo recruited 831 patients. 162 patients were consented for Neo-tAnGo Science, for 3 additional fresh tissue samples to be taken at diagnosis (diag), mid-chemotherapy (CT) and end-CT. Standard methodology was used for PAM 50 subtyping. Results: Fresh tissue samples at diag were received from 123 patients (pts). 45 pts (37%) had 2 additional samples provided (at mid- and end-CT). 57 pts (46%) had 1 additional sample provided (34 at mid-CT, 23 at end-CT). PAM 50 subtyping at diag was as follows: 31 (25%) BASAL; 30 (24%) HER2; 39 (32%) LUM B; 13 (11%) LUM A; 10 (8%) NORMAL-like. Pathological complete response rates (pCR: no disease in breast or axillary nodes, n = 121 pts) differed between PAM 50 subtype at diag (p = 0.04): BASAL 11/31 (35%); HER2 8/30 (27%); LUM B 3/37 (8%); LUM A 1/13 (8%); NORMAL-like 3/10 (30%). Of the 94 pts who were not PAM50 NORMAL-like at diag and had 2+ samples, 42 (45%) ‘shifted to NORMAL-like’. This was associated with slightly higher pCR rates (24% vs 15% who didn’t ‘shift to NORMAL-like’, p = 0.44) and borderline significantly higher rates of pCR or minimal residual disease (MRD

Published

2013

41. Parametrial interstitial brachytherapy for advanced or recurrent pelvic malignancy: the Harvard/Stanford experience

Author

Daniel S. Kapp, Luke Hughes-Davies, and Barbara Silver

Subjects

Adult, medicine.medical_specialty, Adolescent, medicine.medical_treatment, Brachytherapy, Whole-Pelvis, medicine, Humans, Pelvic Neoplasms, Child, Survival rate, Aged, Aged, 80 and over, business.industry, Parametrial, Uterus, Obstetrics and Gynecology, Pelvic cavity, Middle Aged, Surgery, Radiation therapy, medicine.anatomical_structure, Treatment Outcome, Oncology, Child, Preschool, Female, Implant, Neoplasm Recurrence, Local, business, Follow-Up Studies

Abstract

In this study we evaluate the long-term efficacy and safety of transperineal interstitial implants for advanced pelvic malignancy. A total of 139 patients were treated at Stanford University Medical Center and the Joint Center for Radiation Therapy with transperineal template interstitial brachytherapy for locally advanced or recurrent cancers arising in the pelvic organs. Most patients received whole pelvis external beam irradiation to a median dose of 4200 cGy followed by an implant for a median duration of 48 hr to a median implant dose of 3000 cGy (range 600-6000 cGy). Complete follow-up was obtained for 91% of the patients. Median follow-up for survivors is 57 months (range, 10-173 months). The crude disease-free survival rate was 22% at 5 years. The 5-year crude local tumor control rate was 25%. No dose-response relationship could be demonstrated for tumor control or complications. There were no acute treatment-related deaths. Three late deaths were seen which were directly related to treatment. Major bowel complications requiring surgery were seen in 17% of patients without locally recurrent disease, and fistulas were reported in 4% of these patients. We conclude that template parametrial implant brachytherapy offers a modest chance of cure for women with locally advanced pelvic malignancy. However, this treatment causes significant late morbidity.

Published

1995

42. OPTIMA prelim: Optimal personalized treatment of early breast cancer using multiparameter analysis: Preliminary study

Author

Janet A. Dunn, Luke Hughes-Davies, Adele Francis, Peter Canney, Helena M. Earl, Robert Stein, David Cameron, Louise Hiller, Daniel Rea, Sarah E Pinder, Nigel Stallard, Peter Hall, Jenny L Donovan, John M. S. Bartlett, Christopher McCabe, Andreas Makris, Helen B Higgins, Christopher J. Poole, and Adrienne Morgan

Subjects

Gynecology, Oncology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Personalized treatment, Endocrine therapy, medicine.disease, Breast cancer, Internal medicine, medicine, business, Oncotype DX, Early breast cancer

Abstract

TPS665 Background: “Multi-parameter” prognostic tests such as Oncotype DX are increasingly used to identify women with ER +ve HER2 -ve breast cancer treated with endocrine therapy who are unlikely to benefit meaningfully from adjuvant chemotherapy. The supporting evidence for predictive testing is retrospective and is strongest for women with negative nodes. Randomised trials to validate testing are in progress but more evidence is needed, especially for node positive disease. There is early evidence that other multi-parameter tests which are in development have a predictive utility. Methods: OPTIMA will assess the value of multi-parameter tests in a UK population. OPTIMA prelim, the feasibility phase, will recruit 300 patients from May 2012 (with a 200 patient bridging extension to the main study). Eligible patients will have ER +ve HER2 -ve tumours with involved nodes (pN1-2). Patients will be randomised to the standard arm of both chemotherapy and endocrine therapy, or to the “test-directed treatment” arm in which patients will be assigned either the same chemotherapy and endocrine therapy or endocrine therapy only according to the result of an Oncotype DX test. OPTIMA prelim has 3 objectives. (1) To establish whether randomisation to test-directed treatment is acceptable to patients and clinicians. This will be done through qualitative research with in-depth interviews with OPTIMA researchers and by recording and analysing consultations when the trial is discussed with potential participants. (2) Alternative multi-parameter tests will be evaluated on all patients’ tumours and their performance will be compared to Oncotype DX using statistical and cost-effectiveness analysis to select a candidate test(s) appropriate for NHS use to be evaluated in the main trial. (3) The success of the main trial depends on efficient tumour sample collection and analysis to avoid treatment delays. The obstacles to this will be analysed in detail using a sample tracking database. The main study is an efficacy trial of 2-3 arms with the same design but uses tests selected in OPTIMA prelim. It will compare 5-year relapse free survival of test-directed vs. conventional treatment with a non-inferiority hypothesis.

Published

2012

43. BEX2 has a functional interplay with c-Jun/JNK and p65/RelA in breast cancer

Author

Luke Hughes-Davies, Ji Liu, and Ali Naderi

Subjects

Chromatin Immunoprecipitation, Cancer Research, MAP Kinase Kinase 4, Proto-Oncogene Proteins c-jun, Blotting, Western, Transcription Factor RelA, Fluorescent Antibody Technique, Gene Expression, Breast Neoplasms, Enzyme-Linked Immunosorbent Assay, Nerve Tissue Proteins, Biology, lcsh:RC254-282, Cyclin D1, Breast cancer, Cell Line, Tumor, Transcriptional regulation, medicine, Humans, Phosphorylation, Reverse Transcriptase Polymerase Chain Reaction, Research, c-jun, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Enzyme Activation, Gene Expression Regulation, Neoplastic, IκBα, Oncology, Gene Knockdown Techniques, Mutagenesis, Site-Directed, Cancer research, Molecular Medicine, Female, Signal transduction, G1 phase, Signal Transduction

Abstract

Background We have previously demonstrated that BEX2 is differentially expressed in breast tumors and has a significant role in promoting cell survival and growth in breast cancer cells. BEX2 expression protects breast cancer cells against mitochondrial apoptosis and G1 cell cycle arrest. In this study we investigated the transcriptional regulation of BEX2 and feedback mechanisms mediating the cellular function of this gene in breast cancer. Results We found a marked induction of BEX2 promoter by c-Jun and p65/RelA using luciferase reporter assays in MCF-7 cells. Furthermore, we confirmed the binding of c-Jun and p65/RelA to the BEX2 promoter using a chromatin immunoprecipitation assay. Importantly, transfections of c-Jun or p65/RelA in MCF-7 cells markedly increased the expression of BEX2 protein. Overall, these results demonstrate that BEX2 is a target gene for c-Jun and p65/RelA in breast cancer. These findings were further supported by the presence of a strong correlation between BEX2 and c-Jun expression levels in primary breast tumors. Next we demonstrated that BEX2 has a feedback mechanism with c-Jun and p65/RelA in breast cancer. In this process BEX2 expression is required for the normal phosphorylation of p65 and IκBα, and the activation of p65. Moreover, it is necessary for the phosphorylation of c-Jun and JNK kinase activity in breast cancer cells. Furthermore, using c-Jun stable lines we showed that BEX2 expression is required for c-Jun mediated induction of cyclin D1 and cell proliferation. Importantly, BEX2 down-regulation resulted in a significant increase in PP2A activity in c-Jun stable lines providing a possible underlying mechanism for the regulatory effects of BEX2 on c-Jun and JNK. Conclusions This study shows that BEX2 has a functional interplay with c-Jun and p65/RelA in breast cancer. In this process BEX2 is a target gene for c-Jun and p65/RelA and in turn regulates the phosphorylation/activity of these proteins. These suggest that BEX2 is involved in a novel feedback mechanism with significant implications for the biology of breast cancer.

Published

2010

44. Neo-tAnGo: A neoadjuvant randomized phase III trial of epirubicin/cyclophosphamide and paclitaxel ± gemcitabine in the treatment of women with high-risk early breast cancer (EBC): First report of the primary endpoint, pathological complete response (pCR)

Author

Elena Provenzano, Mahesh Iddawela, Tamas Hickish, Helena M. Earl, Nicola Fenwick, Louise Hiller, Luke Hughes-Davies, C Caldas, Anne-Laure Vallier, and Karen McAdam

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, Axillary lymph nodes, Cyclophosphamide, business.industry, medicine.medical_treatment, Gemcitabine, chemistry.chemical_compound, Regimen, medicine.anatomical_structure, Paclitaxel, chemistry, Internal medicine, medicine, Clinical endpoint, business, medicine.drug, Epirubicin

Abstract

522 Background: Neo-tAnGo used a 2-by-2 factorial design, addressing: (i) gemcitabine (G) in a sequential neoadjuvant chemotherapy (CT) regimen of epirubicin/cyclophosphamide (EC) and paclitaxel (T); and (ii) the sequencing of these treatment components (EC then T ± G versus T ± G then EC). Methods: Patients (Pts) with early breast cancer (T2 tumours or above) were randomised to EC then T, T then EC, EC then TG or TG then EC. All components were given x 4 cycles. (E= 90 mg/m2 day (d)1 every (q) 21d; C = 600 mg/m2 d1 q21d; T = 175 mg/m2 d1 q14d; G = 2,000 mg/m2 d1 q14d.) The primary endpoint was pCR, defined as absence of invasive disease in the breast and axillary lymph nodes. 800 pts were required to detect 10% differences in the primary endpoint pCR rates, at the 5% (2-sided) significance level with 85% power. Stratification was by age, inflammatory/locally advanced disease, tumour size, clinical involvement of axillary nodes and oestrogen receptor (ER) status. Results: Between January 2005 and September 2007, 831 pts were randomised by 88 consultants from 57 UK centres. Characteristics were balanced across groups: 63% [Table: see text]

Published

2009

45. Fluorouracil and folinic acid in colon cancer

Author

John Rescigno, Silvia Marsoni, and Luke Hughes-Davies

Subjects

Oncology, medicine.medical_specialty, Chemotherapy, Disease free survival, business.industry, Colorectal cancer, medicine.medical_treatment, General Medicine, medicine.disease, Folinic acid, Text mining, Fluorouracil, Internal medicine, medicine, business, Adjuvant, medicine.drug

Published

1995

46. Management and long-term outcome of patients presenting with clinical stage IA–IIB Hodgkins disease with extensive thoracic involvement

Author

Luke Hughes-Davies, Peter Mauch, and Barbara Silver

Subjects

Cancer Research, medicine.medical_specialty, Pediatrics, Radiation, business.industry, Disease, Outcome (game theory), Surgery, Term (time), Oncology, medicine, Radiology, Nuclear Medicine and imaging, Stage (cooking), business

Published

1994

47. Fourniers gangrene: A hazard of chemotherapy in AIDS

Author

Margaret F. Spittle, Luke Hughes-Davies, and P. Murray

Subjects

medicine.medical_specialty, Chemotherapy, business.industry, General surgery, medicine.medical_treatment, medicine.disease, Hazard, Surgery, Oncology, Acquired immunodeficiency syndrome (AIDS), medicine, Radiology, Nuclear Medicine and imaging, business, Fourniers gangrene

Published

1991

48. Radiosensitivity in AIDS patients

Author

Teresa E Young, Luke Hughes-Davies, and Margaret F Spittle

Subjects

Oncology, medicine.medical_specialty, Aids patients, business.industry, Internal medicine, medicine, General Medicine, Radiosensitivity, business

Published

1991

49. Effects of the addition of gemcitabine, and paclitaxel-first sequencing, in neoadjuvant sequential epirubicin, cyclophosphamide, and paclitaxel for women with high-risk early breast cancer (Neo-tAnGo): an open-label, 2×2 factorial randomised phase 3 trial

Author

Tamas Hickish, Luke Hughes-Davies, Jennie Young, Gordon C. Wishart, Anne-Laure Vallier, Ioannis Gounaris, Anthony Skene, Susan Dean, Carlos Caldas, Mahesh Iddawela, Janet A. Dunn, Stephen Houston, Robert W. Laing, Elena Provenzano, Helena M. Earl, Louise Hiller, Karen McAdam, Mark Harries, Stephen Chan, Jean Abraham, Nicola Fenwick, J. Christopher Gallagher, and Diana Ritchie

Subjects

Oncology, medicine.medical_specialty, Time Factors, Anthracycline, Bevacizumab, Cyclophosphamide, Paclitaxel, medicine.medical_treatment, Breast Neoplasms, Kaplan-Meier Estimate, Deoxycytidine, Disease-Free Survival, Drug Administration Schedule, Risk Factors, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Biomarkers, Tumor, Humans, skin and connective tissue diseases, Epirubicin, Proportional Hazards Models, Chemotherapy, Taxane, business.industry, Middle Aged, Gemcitabine, Neoadjuvant Therapy, United Kingdom, Tumor Burden, Logistic Models, Treatment Outcome, Docetaxel, Chemotherapy, Adjuvant, Lymphatic Metastasis, Multivariate Analysis, Female, business, medicine.drug

Abstract

SummaryBackgroundAnthracyclines and taxanes have been the standard neoadjuvant chemotherapies for breast cancer in the past decade. We aimed to assess safety and efficacy of the addition of gemcitabine to accelerated paclitaxel with epirubicin and cyclophosphamide, and also the effect of sequencing the blocks of epirubicin and cyclophosphamide and paclitaxel (with or without gemcitabine).MethodsIn our randomised, open-label, 2×2 factorial phase 3 trial (Neo-tAnGo), we enrolled women (aged >18 years) with newly diagnosed breast cancer (tumour size >20 mm) at 57 centres in the UK. Patients were randomly assigned via a central randomisation procedure to epirubicin and cyclophosphamide then paclitaxel (with or without gemcitabine) or paclitaxel (with or without gemcitabine) then epirubicin and cyclophosphamide. Four cycles of each component were given. The primary endpoint was pathological complete response (pCR), defined as absence of invasive cancer in the breast and axillary lymph nodes. This study is registered with EudraCT (2004-002356-34), ISRCTN (78234870), and ClinicalTrials.gov (NCT00070278).FindingsBetween Jan 18, 2005, and Sept 28, 2007, we randomly allocated 831 participants; 207 received epirubicin and cyclophosphamide then paclitaxel; 208 were given paclitaxel then epirubicin and cyclophosphamide; 208 had epirubicin and cyclophosphamide followed by paclitaxel and gemcitabine; and 208 received paclitaxel and gemcitabine then epirubicin and cyclophosphamide. 828 patients were eligible for analysis. Median follow-up was 47 months (IQR 37–51). 207 (25%) patients had inflammatory or locally advanced disease, 169 (20%) patients had tumours larger than 50 mm, 413 (50%) patients had clinical involvement of axillary nodes, 276 (33%) patients had oestrogen receptor (ER)-negative disease, and 191 (27%) patients had HER2-positive disease. Addition of gemcitabine did not increase pCR: 70 (17%, 95% CI 14–21) of 404 patients in the epirubicin and cyclophosphamide then paclitaxel group achieved pCR compared with 71 (17%, 14–21) of 408 patients who received additional gemcitabine (p=0·98). Receipt of a taxane before anthracycline was associated with improved pCR: 82 (20%, 95% CI 16–24) of 406 patients who received paclitaxel with or without gemcitabine followed by epirubicin and cyclophosphamide achieved pCR compared with 59 (15%, 11–18) of 406 patients who received epirubicin and cyclophosphamide first (p=0·03). Grade 3 toxicities were reported at expected levels: 173 (21%) of 812 patients who received treatment and had full treatment details had grade 3 neutropenia, 66 (8%) had infection, 41 (5%) had fatigue, 41 (5%) had muscle and joint pains, 37 (5%) had nausea, 36 (4%) had vomiting, 34 (4%) had neuropathy, 23 (3%) had transaminitis, 16 (2%) had acute hypersensitivity, and 20 (2%) had a rash. 86 (11%) patients had grade 4 neutropenia and 3 (