Medicine (St Vincent's) - Research Publications

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Start date: 1980 × Author: Zalcberg, John ×

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    Pre- and Postoperative Capecitabine Without or With Oxaliplatin in Locally Advanced Rectal Cancer: PETACC 6 Trial by EORTC GITCG and ROG, AIO, AGITG, BGDO, and FFCD
    Schmoll, H-J ; Stein, A ; Van Cutsem, E ; Price, T ; Hofheinz, RD ; Nordlinger, B ; Daisne, J-F ; Janssens, J ; Brenner, B ; Reinel, H ; Hollerbach, S ; Caca, K ; Fauth, F ; Hannig, CV ; Zalcberg, J ; Tebbutt, N ; Mauer, ME ; Marreaud, S ; Lutz, MP ; Haustermans, K (AMER SOC CLINICAL ONCOLOGY, 2021-01-01)
    PURPOSE: The PETACC 6 trial investigates whether the addition of oxaliplatin to preoperative capecitabine-based chemoradiation and postoperative capecitabine improves disease-free survival (DFS) in locally advanced rectal cancer. METHODS: Between November 2008 and September 2011, patients with rectal adenocarcinoma within 12 cm from the anal verge, T3/4 and/or node positive, were randomly assigned to 5 weeks preoperative capecitabine-based chemoradiation (45-50.4 Gy) followed by six cycles of adjuvant capecitabine, both without (control arm, 1) or with (experimental arm, 2) oxaliplatin. The primary end point was improvement of 3-year DFS by oxaliplatin from 65% to 72% (hazard ratio [HR], 0.763). RESULTS: A total of 1,094 patients were randomly assigned (intention to treat), and 1,068 eligible patients started their allocated treatment (arm 1, 543; arm 2, 525), with completion of protocol treatment in 68% (arm 1) v 54% (arm 2). A higher rate of grade 3/4 adverse events was reported in the experimental arm (14.4% v 37.3% and 23.4% v 46.6% for neoadjuvant and adjuvant treatment, respectively). At a median follow-up of 68 months (interquartile range, 58-74 months), 157 and 156 DFS events were observed in arms 1 and 2, respectively (adjusted HR, 1.02; 95% CI, 0.82 to 1.28; P = .835). Three-year DFS rate was not different, with 76.5% (95% CI, 72.7% to 79.9%) in arm 1, which is higher than anticipated, and 75.8% (95% CI, 71.9% to 79.3%) in arm 2. The 7-year DFS and overall survival (OS) rates were not different as well, with DFS of 66.1% v 65.5% (HR, 1.02) and OS of 73.5% v 73.7% (HR, 1.19) in arms 1 and 2, respectively. Subgroup analyses revealed heterogeneity in treatment effect according to German versus non-German site location, without detectable confounding factors in multivariable analysis. CONCLUSION: The addition of oxaliplatin to preoperative capecitabine-based chemoradiation and postoperative adjuvant chemotherapy impairs tolerability and feasibility and does not improve efficacy.
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    Putting the "good" into Good Clinical Practice
    Symons, T ; Webb, S ; Zalcberg, JR (WILEY, 2021-02)
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    Do all services provided as part of a clinical trial require research ethics and governance review?
    Kenner, J ; Zalcberg, JR (Wiley, 2017-10)
    Appropriate ethical oversight underpins the conduct of all clinical trials in Australia. In addition, clinical trials require a suitable approach to research governance in order to ensure that research is appropriately governed. However, such governance processes are often onerous and time-consuming and are not required when trial practices are more appropriately understood as standard of care clinical services.
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    Clinical Benefit of Ripretinib Dose Escalation After Disease Progression in Advanced Gastrointestinal Stromal Tumor: An Analysis of the INVICTUS Study.
    Zalcberg, JR ; Heinrich, MC ; George, S ; Bauer, S ; Schöffski, P ; Serrano, C ; Gelderblom, H ; Jones, RL ; Attia, S ; D'Amato, G ; Chi, P ; Reichardt, P ; Somaiah, N ; Meade, J ; Reichert, V ; Shi, K ; Sherman, ML ; Ruiz-Soto, R ; von Mehren, M ; Blay, J-Y (Oxford University Press (OUP), 2021-11)
    BACKGROUND: Ripretinib 150 mg once daily (QD) is indicated for advanced gastrointestinal stromal tumors (GISTs) as at least fourth-line therapy. In INVICTUS, ripretinib intrapatient dose escalation (IPDE) to 150 mg b.i.d. was allowed after progressive disease (PD) on 150 mg QD by blinded independent central review using modified RECIST 1.1. We report the efficacy and safety of ripretinib IPDE to 150 mg b.i.d. after PD among patients randomized to ripretinib 150 mg QD in the INVICTUS study. MATERIALS AND METHODS: Tumor imaging was performed every 28-day cycle for the first four cycles in the ripretinib 150 mg QD period and then every other cycle, including the 150 mg b.i.d. PERIOD: Among the ripretinib IPDE patients, progression-free survival (PFS)1 was the time from randomization until PD; PFS2 was the time from the first dose of ripretinib 150 mg b.i.d. to PD or death. RESULTS: Among 43 ripretinib IPDE patients, median PFS1 was 4.6 months (95% confidence interval [CI], 2.7-6.4) and median PFS2 was 3.7 months (95% CI, 3.1-5.3). Median overall survival was 18.4 months (95% CI, 14.5-not estimable). Ripretinib 150 mg b.i.d. (median duration of treatment 3.7 months) was well tolerated with new or worsening grade 3-4 treatment-emergent adverse events (TEAEs) of anemia in six (14%) and abdominal pain in three (7%) patients. Ripretinib 150 mg b.i.d. was discontinued because of TEAEs in seven (16%) patients. CONCLUSION: Ripretinib 150 mg b.i.d. after PD on 150 mg QD may provide additional clinically meaningful benefit with an acceptable safety profile in patients with at least fourth-line GISTs. IMPLICATIONS FOR PRACTICE: Of the 85 patients with advanced gastrointestinal stromal tumor having received at least three prior anticancer therapies randomized to ripretinib 150 mg once daily (QD) in the phase III INVICTUS study, 43 underwent ripretinib intrapatient dose escalation (IPDE) to 150 mg b.i.d. after progressive disease (PD). Median progression-free survival was 4.6 months before and 3.7 months after ripretinib IPDE. The safety profile of ripretinib 150 mg b.i.d. was acceptable. These findings indicate ripretinib IPDE to 150 mg b.i.d. may provide additional clinical benefit in patients with PD on ripretinib 150 mg QD, for whom limited treatment options exist.
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    Improving regional access: Phase 1 teletrials in the era of COVID-19.
    Gaughran, G ; Zalcberg, J ; Hawkins, C-A ; Shackleton, M ; Voskoboynik, M (Wiley, 2021-08)
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    Genomic Risk Prediction for Breast Cancer in Older Women
    Lacaze, P ; Bakshi, A ; Riaz, M ; Orchard, SG ; Tiller, J ; Neumann, JT ; Carr, PR ; Joshi, AD ; Cao, Y ; Warner, ET ; Manning, A ; Nguyen-Dumont, T ; Southey, MC ; Milne, RL ; Ford, L ; Sebra, R ; Schadt, E ; Gately, L ; Gibbs, P ; Thompson, BA ; Macrae, FA ; James, P ; Winship, I ; McLean, C ; Zalcberg, JR ; Woods, RL ; Chan, AT ; Murray, AM ; McNeil, JJ (MDPI, 2021-07)
    Genomic risk prediction models for breast cancer (BC) have been predominantly developed with data from women aged 40-69 years. Prospective studies of older women aged ≥70 years have been limited. We assessed the effect of a 313-variant polygenic risk score (PRS) for BC in 6339 older women aged ≥70 years (mean age 75 years) enrolled into the ASPREE trial, a randomized double-blind placebo-controlled clinical trial investigating the effect of daily 100 mg aspirin on disability-free survival. We evaluated incident BC diagnoses over a median follow-up time of 4.7 years. A multivariable Cox regression model including conventional BC risk factors was applied to prospective data, and re-evaluated after adding the PRS. We also assessed the association of rare pathogenic variants (PVs) in BC susceptibility genes (BRCA1/BRCA2/PALB2/CHEK2/ATM). The PRS, as a continuous variable, was an independent predictor of incident BC (hazard ratio (HR) per standard deviation (SD) = 1.4, 95% confidence interval (CI) 1.3-1.6) and hormone receptor (ER/PR)-positive disease (HR = 1.5 (CI 1.2-1.9)). Women in the top quintile of the PRS distribution had over two-fold higher risk of BC than women in the lowest quintile (HR = 2.2 (CI 1.2-3.9)). The concordance index of the model without the PRS was 0.62 (95% CI 0.56-0.68), which improved after addition of the PRS to 0.65 (95% CI 0.59-0.71). Among 41 (0.6%) carriers of PVs in BC susceptibility genes, we observed no incident BC diagnoses. Our study demonstrates that a PRS predicts incident BC risk in women aged 70 years and older, suggesting potential clinical utility extends to this older age group.
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    Impact of geography on prognostic outcomes of 21,509 patients with metastatic colorectal cancer enrolled in clinical trials: an ARCAD database analysis.
    Yin, J ; Dawood, S ; Cohen, R ; Meyers, J ; Zalcberg, J ; Yoshino, T ; Seymour, M ; Maughan, T ; Saltz, L ; Van Cutsem, E ; Venook, A ; Schmoll, H-J ; Goldberg, R ; Hoff, P ; Hecht, JR ; Hurwitz, H ; Punt, C ; Diaz Rubio, E ; Koopman, M ; Cremolini, C ; Heinemann, V ; Tournigard, C ; Bokemeyer, C ; Fuchs, C ; Tebbutt, N ; Souglakos, J ; Doulliard, J-Y ; Kabbinavar, F ; Chibaudel, B ; de Gramont, A ; Shi, Q ; Grothey, A ; Adams, R (SAGE Publications, 2021)
    BACKGROUND: Benchmarking international cancer survival differences is necessary to evaluate and improve healthcare systems. Our aim was to assess the potential regional differences in outcomes among patients with metastatic colorectal cancer (mCRC) participating in international randomized clinical trials (RCTs). DESIGN: Countries were grouped into 11 regions according to the World Health Organization and the EUROCARE model. Meta-analyses based on individual patient data were used to synthesize data across studies and regions and to conduct comparisons for outcomes in a two-stage random-effects model after adjusting for age, sex, performance status, and time period. We used mCRC patients enrolled in the first-line RCTs from the ARCAD database, which provided enrolling country information. There were 21,509 patients in 27 RCTs included across the 11 regions. RESULTS: Main outcomes were overall survival (OS) and progression-free survival (PFS). Compared with other regions, patients from the United Kingdom (UK) and Ireland were proportionaly over-represented, older, with higher performance status, more frequently male, and more commonly not treated with biological therapies. Cohorts from central Europe and the United States (USA) had significantly longer OS compared with those from UK and Ireland (p = 0.0034 and p < 0.001, respectively), with median difference of 3-4 months. The survival deficits in the UK and Ireland cohorts were, at most, 15% at 1 year. No evidence of a regional disparity was observed for PFS. Among those treated without biological therapies, patients from the UK and Ireland had shorter OS than central Europe patients (p < 0.001). CONCLUSIONS: Significant international disparities in the OS of cohorts of mCRC patients enrolled in RCTs were found. Survival of mCRC patients included in RCTs was consistently lower in the UK and Ireland regions than in central Europe, southern Europe, and the USA, potentially attributed to greater overall population representation, delayed diagnosis, and reduced availability of therapies.
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    Implementation of the Australasian Teletrial Model: Lessons from practice
    Sabesan, S ; Zalcberg, J ; Underhill, C ; Zielinski, R ; Burbury, K ; Ansari, Z ; Rainey, N ; Collins, I ; Osbourne, R ; Sanmugarajah, J ; Joshua, A ; Honeyball, F ; Poxton, M ; Gebbie, C ; Marsh, SJ ; Lusa, R ; Johnson, T ; Garbutt, A ; Bransdon, M ; Richmond, S ; Waye, R ; Cross, H ; Kent, R ; Darch, J ; Brown, A (WILEY, 2019-11)