Medicine (St Vincent's) - Research Publications

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Start date: 2020 × End date: 2022 × Author: Tam, Constantine × Type: Journal Article ×

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    PRELIMINARY SAFETY DATA FROM PATIENTS (PTS) WITH RELAPSED/REFRACTORY (R/R) B‐CELL MALIGNANCIES TREATED WITH THE NOVEL B‐CELL LYMPHOMA 2 (BCL2) INHIBITOR BGB‐11417
    Cheah, CY ; Verner, E ; Tam, CS ; Hilger, J ; Gao, Y ; Huang, J ; Simpson, D ; Opat, S (Wiley, 2021-06)
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    Fitness criteria for Australian patients referred for chimeric antigen receptor T-cell therapy
    Tam, CS ; Ho, PJ ; Purtill, D ; Blyth, E ; Butler, J ; Dickinson, M ; Harrison, S (WILEY, 2022-08)
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    Current perspectives regarding SARS-CoV-2 vaccination in chronic lymphocytic leukemia
    Molica, S ; Tam, C ; Polliack, A (WILEY, 2022-08)
    In immunocompetent people, the mRNA vaccines BNT162b2 and mRNA-1273 have been shown to be safe and effective against coronavirus disease of 2019 (COVID-19). However, results of cohort studies and meta-analyses have indicated that the degree of humoral response to SARS-CoV-2 vaccines in patients with chronic lymphocytic leukemia (CLL) appears to be lower than that observed in the general population. These inadequate responses are mainly related to the disease itself and to the immunosuppressive effect of therapies administered. In the specific context of CLL, enrolling patients with sub-optimal vaccine-response in pivotal vaccine trials could be considered as an appropriate approach to improve response to the COVID-19 vaccine. These clinical trials should also address the issues of regularity and timing of vaccine booster doses or re-vaccinations, especially in patients undergoing therapy with pathway-targeting agents and anti-CD20 monoclonal antibodies. However, since hypogammaglobulinemia is a serious consequence of CLL, patients who do not have a detectable antibody response should be natural candidates for preventive antibody therapy.
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    Recommendation for TP53 mutation testing in newly diagnosed mantle cell lymphoma: a statement from working groups sponsored by the Victorian Comprehensive Cancer Centre
    Tam, CS ; Gregory, GP ; Ku, M ; Fleming, S ; Handunnetti, SM ; Lee, D ; Walker, P ; Perkins, A ; Lew, TE ; Sirdesai, S ; Chua, CC ; Gilbertson, M ; Lasica, M ; Anderson, MA ; Renwick, W ; Grigg, A ; Patil, S ; Opat, S ; Friebe, A ; Cooke, R ; De Boer, J ; Spencer, A ; Ritchie, D ; Agarwal, R ; Blombery, P (WILEY, 2022-07)
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    Cytomegalovirus DNAemia and disease: current-era epidemiology, clinical characteristics and outcomes in cancer patients other than allogeneic haemopoietic transplantation
    Tay, KH ; Slavin, MA ; Thursky, KA ; Coussement, J ; Worth, LJ ; Teh, BW ; Khot, A ; Tam, CS ; Yong, MK (WILEY, 2022-10)
    BACKGROUND: High-intensity chemotherapy and advances in novel immunotherapies have seen the emergence of cytomegalovirus (CMV) infections in cancer patients other than allogeneic haemopoietic cell transplantation (HCT). Aim To evaluate the epidemiology, clinical characteristics and outcomes of CMV infection in this population. METHODS: A retrospective review of cancer patients other than allogeneic HCT who had CMV DNAemia and/or disease from July 2013 till May 2020 at a quaternary cancer centre was performed. RESULTS: Of 11 485 cancer patients who underwent treatment during this period, 953 patients had CMV DNA testing performed and 238 of them had CMV DNAemia. After excluding patients with allogeneic HCT, 62 patients with CMV DNAemia were identified, of whom 10 had concurrent CMV disease. The most frequent underlying malignancies were B-cell lymphoproliferative disease (LPD) (31%; 19/62), T-cell LPD (21%; 13/62), chronic lymphocytic leukaemia (11%; 7/62) and multiple myeloma (10%; 6/62). Most patients had lymphopenia (77%; 48/62), multiple cancer therapies (63%; 39/62 received ≥2 previous therapies), co-infection (56%; 35/62 had ≥1 co-infection) and corticosteroid therapy (48%; 30/62) within 1 month before CMV diagnosis. CMV DNAemia and disease were observed in patients receiving novel immunotherapies, including bispecific antibody therapy, chimeric-antigen receptor T-cell therapy and immune checkpoint inhibitors. CONCLUSION: Patients with haematological malignancy, particularly B-cell LPD, T-cell LPD, chronic lymphocytic leukaemia and multiple myeloma, were frequently identified to have CMV DNAemia and disease. Lymphopenia, multiple cancer therapies, co-infection and recent receipt of systemic corticosteroids were also commonly observed. Future studies are necessary to determine optimal identification and management of CMV in these patients.
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    Improving outcomes for patients with lymphoma: design and development of the Australian and New Zealand Lymphoma and Related Diseases Registry
    Anderson, MA ; Berkahn, L ; Cheah, C ; Dickinson, M ; Gandhi, MK ; Giri, P ; Hawkes, EA ; Johnston, A ; Keane, C ; McQuilten, ZK ; Mulligan, SP ; Opat, S ; Talaulikar, D ; Trotman, J ; Williams, J ; Wood, EM ; Armytage, T ; Barraclough, A ; Carradice, D ; Chong, G ; Cochrane, T ; Hamad, N ; Ku, M ; Lee, D ; Morgan, S ; Mutsando, H ; Narayana, M ; Prince, HM ; Ratnasingam, S ; Wight, J ; Badoux, X ; Cull, G ; Kuss, B ; Marlton, P ; Tam, C ; Casan, J ; Cushion, T ; Tedjaseputra, A ; Birch, S ; Brown, C ; Ellis, D ; Harvey, Y ; Hitchins, S ; Jain, S ; Jessup, P ; Juneja, S ; Kearney, D ; Kumar, B ; Lade, S ; Lee, K ; Leslie, C ; Long, E ; Morey, A ; Nath, L ; Norris, D ; Parker, A ; Parry, J ; Chen, FP-Y ; Chung, E ; Morison, J ; Rowsell, L ; St George, G ; Thu, C ; Waters, N ; Wellard, C ; Zheng, M (BMC, 2022-10-10)
    BACKGROUND: Lymphoma is a malignancy of lymphocytes and lymphoid tissues comprising a heterogeneous group of diseases, with up to 80 entities now described. Lymphoma is the 6th most common cancer in Australia, affecting patients of all ages, with rising incidence rates. With the proliferation of efficacious novel agents, therapeutic strategies are increasingly diverse and survival is improving. There is a clear need for contemporary robust and detailed data on diagnostic, investigational and management strategies for this disease in Australia, New Zealand and worldwide, to inform and benchmark local and international standards of care. Clinical quality registries can provide these data, and support development of strategies to address variations in management, including serving as platforms for clinical trials and other research activities. The Lymphoma and Related Diseases Registry (LaRDR) was developed to capture details of patient demographics, disease characteristics, and management throughout their disease course and therapy and to develop outcome benchmarks nationally and internationally for lymphoma. This report describes the aims, development and implementation of the LaRDR, as well as challenges addressed in the process. METHODS: The LaRDR was established in 2016 as a multicentre, collaborative project at sites across Australia with a secure online database which collects prospective data on patients with a new diagnosis of lymphoma or chronic lymphocytic leukaemia (CLL). LaRDR development required multidisciplinary participation including specialist haematology, information technology, and biostatistical support, as well as secure funding. Here we describe the database development, data entry, ethics approval process, registry governance and support for participating sites and the coordinating centre. RESULTS: To date more than 5,300 patients have been enrolled from 28 sites in Australia and New Zealand. Multiple challenges arose during the development, which we describe, along with approaches used to overcome them. Several confirmed international collaborations are now in place, and the registry is providing valuable data for clinicians, researchers, industry and government, including through presentations of results at major national and international conferences. CONCLUSION: Challenges in establishing the LaRDR have been successfully overcome and the registry is now a valuable resource for lymphoma clinicians, researchers, health economists and others in Australia, New Zealand and globally.
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    Consensus opinion from an international group of experts on measurable residual disease in hairy cell leukemia
    Ravandi, F ; Kreitman, RJ ; Tiacci, E ; Andritsos, L ; Banerji, V ; Barrientos, JC ; Bhat, SA ; Blachly, JS ; Broccoli, A ; Call, T ; Chihara, D ; Dearden, C ; Demeter, J ; Dietrich, S ; Else, M ; Epperla, N ; Falini, B ; Forconi, F ; Gladstone, DE ; Gozzetti, A ; Iyengar, S ; Johnston, JB ; Jorgensen, J ; Juliusson, G ; Lauria, F ; Lozanski, G ; Parikh, SA ; Park, JH ; Polliack, A ; Quest, G ; Robak, T ; Rogers, KA ; Saven, A ; Seymour, JF ; Tadmor, T ; Tallman, MS ; Tam, CS ; Thompson, PA ; Troussard, X ; Zent, CS ; Zenz, T ; Zinzani, PL ; Woermann, B ; Rai, K ; Grever, M (SPRINGERNATURE, 2022-12-13)
    A significant body of literature has been generated related to the detection of measurable residual disease (MRD) at the time of achieving complete remission (CR) in patients with hairy cell leukemia (HCL). However, due to the indolent nature of the disease as well as reports suggesting long-term survival in patients treated with a single course of a nucleoside analog albeit without evidence of cure, the merits of detection of MRD and attempts to eradicate it have been debated. Studies utilizing novel strategies in the relapse setting have demonstrated the utility of achieving CR with undetectable MRD (uMRD) in prolonging the duration of remission. Several assays including immunohistochemical analysis of bone marrow specimens, multi-parameter flow cytometry and molecular assays to detect the mutant BRAF V600E gene or the consensus primer for the immunoglobulin heavy chain gene (IGH) rearrangement have been utilized with few comparative studies. Here we provide a consensus report on the available data, the potential merits of MRD assessment in the front-line and relapse settings and recommendations on future role of MRD assessment in HCL.
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    Single-cell multiomics reveal the scale of multilayered adaptations enabling CLL relapse during venetoclax therapy
    Thijssen, R ; Tian, L ; Anderson, MA ; Flensburg, C ; Jarratt, A ; Garnham, AL ; Jabbari, JS ; Peng, H ; Lew, TE ; Teh, CE ; Gouil, Q ; Georgiou, A ; Tan, T ; Djajawi, TM ; Tam, CS ; Seymour, JF ; Blombery, P ; Gray, DHD ; Majewski, IJ ; Ritchie, ME ; Roberts, AW ; Huang, DCS (AMER SOC HEMATOLOGY, 2022-11-17)
    Venetoclax (VEN) inhibits the prosurvival protein BCL2 to induce apoptosis and is a standard therapy for chronic lymphocytic leukemia (CLL), delivering high complete remission rates and prolonged progression-free survival in relapsed CLL but with eventual loss of efficacy. A spectrum of subclonal genetic changes associated with VEN resistance has now been described. To fully understand clinical resistance to VEN, we combined single-cell short- and long-read RNA-sequencing to reveal the previously unappreciated scale of genetic and epigenetic changes underpinning acquired VEN resistance. These appear to be multilayered. One layer comprises changes in the BCL2 family of apoptosis regulators, especially the prosurvival family members. This includes previously described mutations in BCL2 and amplification of the MCL1 gene but is heterogeneous across and within individual patient leukemias. Changes in the proapoptotic genes are notably uncommon, except for single cases with subclonal losses of BAX or NOXA. Much more prominent was universal MCL1 gene upregulation. This was driven by an overlying layer of emergent NF-κB (nuclear factor kappa B) activation, which persisted in circulating cells during VEN therapy. We discovered that MCL1 could be a direct transcriptional target of NF-κB. Both the switch to alternative prosurvival factors and NF-κB activation largely dissipate following VEN discontinuation. Our studies reveal the extent of plasticity of CLL cells in their ability to evade VEN-induced apoptosis. Importantly, these findings pinpoint new approaches to circumvent VEN resistance and provide a specific biological justification for the strategy of VEN discontinuation once a maximal response is achieved rather than maintaining long-term selective pressure with the drug.
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    Development of a distributed international patient data registry for hairy cell leukemia
    Andritsos, LA ; Anghelina, M ; Neal, J ; Blachly, JS ; Mathur, P ; Lele, O ; Dearden, C ; Iyengar, S ; Cross, M ; Zent, CS ; Rogers, KA ; Epperla, N ; Lozanski, G ; Oakes, CC ; Kraut, E ; Ruppert, AS ; Zhao, Q ; Bhat, SA ; Forconi, F ; Banerji, V ; Handunnetti, S ; Tam, CS ; Seymour, JF ; Else, M ; Kreitman, RJ ; Saven, A ; Call, T ; Parikh, SA ; Ravandi, F ; Johnston, JB ; Tiacci, E ; Troussard, X ; Tallman, MS ; Dietrich, S ; Tadmor, T ; Gozzetti, A ; Zinzani, PL ; Robak, T ; Quest, G ; Demeter, J ; Rai, K ; Fernandez, SA ; Grever, M (TAYLOR & FRANCIS LTD, 2022-11-10)
    Hairy cell leukemia (HCL) is a rare lymphoproliferative disorder, comprising only 2% of all leukemias. The Hairy Cell Leukemia Foundation (HCLF) has developed a patient data registry to enable investigators to better study the clinical features, treatment outcomes, and complications of patients with HCL. This system utilizes a centralized registry architecture. Patients are enrolled at HCL Centers of Excellence (COE) or via a web-based portal. All data are de-identified, which reduces regulatory burden and increases opportunities for data access and re-use. To date, 579 patients have been enrolled in the registry. Efforts are underway to engage additional COE's to expand access to patients across the globe. This international PDR will enable researchers to study outcomes in HCL in ways not previously possible due to the rarity of the disease and will serve as a platform for future prospective research.
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    SOHO State of the Art Updates and Next Questions | Mechanisms of Resistance to BCL2 Inhibitor Therapy in Chronic Lymphocytic Leukemia and Potential Future Therapeutic Directions
    Bennett, R ; Thompson, E ; Tam, C (CIG MEDIA GROUP, LP, 2022-11)
    Chronic lymphocytic leukaemia (CLL) constitutively overexpresses B-cell lymphoma 2 (BCL2) with consequent dysregulation of intrinsic apoptosis leading to abnormal cellular survival. Therapeutic use of BCL2 inhibitors (BCL2i, eg, venetoclax) in CLL, as both continuous monotherapy or in fixed duration combination, has translated scientific rationale into clinical benefit with significant rates of complete responses, including those without detectable minimal residual disease. Unlike with chemotherapy, response rates to venetoclax do not appear to be influenced by pre-existing chromosomal abnormalities or somatic mutations present, although the duration of response observed remains shorter for those with traditional higher risk genetic aberrations. This review seeks to describe both the disease factors that influence primary venetoclax sensitivity/resistance and those resistance mechanisms that may be acquired secondary to BCL2i therapy in CLL. Baseline venetoclax-sensitivity or -resistance is influenced by the expression of BCL2 relative to other BCL2 family member proteins, microenvironmental factors including nodal T-cell stimulation, and tumoral heterogeneity. With selection pressure applied by continuous venetoclax exposure, secondary resistance mechanisms develop in oligoclonal fashion. Those mechanisms described include acquisition of BCL2 variants, dynamic aberrations of alternative BCL2 family proteins, and mutations affecting both BAX and other BH3 proteins. In view of the resistance described, this review also proposes future applications of BCL2i therapy in CLL and potential means by which BCL2i-resistance may be abrogated.