Molecular determinants of outcomes in relapsed or refractory mantle cell lymphoma treated with ibrutinib or temsirolimus in the MCL3001 (RAY) trial

被引:0
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作者
Ciara L. Freeman
Prasath Pararajalingam
Ling Jin
Sriram Balasubramanian
Aixiang Jiang
Wendan Xu
Michael Grau
Myroslav Zapukhlyak
Merrill Boyle
Brendan Hodkinson
Michael Schaffer
Christopher Enny
Sanjay Deshpande
Steven Sun
Jessica Vermeulen
Ryan D. Morin
David W. Scott
Georg Lenz
机构
[1] Centre for Lymphoid Cancer,Department of Molecular Biology and Biochemistry
[2] BC Cancer,Medical Department A for Hematology, Oncology and Pneumology
[3] Simon Fraser University,Oncology Translational Research
[4] University Hospital Münster,Department of Pathology and Laboratory Medicine
[5] Janssen Research & Development,Oncology Translational Research
[6] University of British Columbia,Clinical Oncology
[7] Janssen Research & Development,Clinical Biostats
[8] Janssen Research & Development,Clinical Oncology
[9] Janssen Research & Development,Blood and Marrow Transplant and Cellular Immunotherapy, H. Lee Moffitt Cancer Centre and Research Institute, Morsani College of Medicine
[10] Janssen Research & Development,undefined
[11] University of South Florida,undefined
来源
Leukemia | 2022年 / 36卷
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摘要
Mantle cell lymphoma (MCL) is a rare, incurable lymphoma subtype characterized by heterogeneous outcomes. To better understand the clinical behavior and response to treatment, predictive biomarkers are needed. Using residual archived material from patients enrolled in the MCL3001 (RAY) study, we performed detailed analyses of gene expression and targeted genetic sequencing. This phase III clinical trial randomized patients with relapsed or refractory MCL to treatment with either ibrutinib or temsirolimus. We confirmed the prognostic capability of the gene expression proliferation assay MCL35 in this cohort treated with novel agents; it outperformed the simplified MCL International Prognostic Index in discriminating patients with different outcomes. Regardless of treatment arm, our data demonstrated that this assay captures the risk conferred by known biological factors, including increased MYC expression, blastoid morphology, aberrations of TP53, and truncated CCND1 3′ untranslated region. We showed the negative impact of BIRC3 mutations/deletions on outcomes in this cohort and identified that deletion of chromosome 8p23.3 also negatively impacts survival. Restricted to patients with deletions/alterations in TP53, ibrutinib appeared to abrogate the deleterious impact on outcome. These data illustrate the potential to perform a molecular analysis of predictive biomarkers on routine patient samples that can meaningfully inform clinical practice.
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页码:2479 / 2487
页数:8
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