PO.CL01.08 · 临床研究

Baseline cfDNA fragmentomics identifies multiple myeloma patients at risk of early progression

编号 2597 展板 16 时间 4/20 09:00–12:00 区域 Section 46 主讲 Dor Abelman, BS
分会场 Liquid Biopsies: Circulating Nucleic Acids 2
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作者与单位

Dor David Abelman1, Jenna Eagles2, Aimee Wong3, Saumil Shah4, Jeffrey Bruce2, Stephanie Pedersen2, David S. Scott2, Cecilia Bonolo de Campos2, Signy Chow5, Darrell White6, Irwindeed Sandhu7, Kevin Song8, Esteban Braggio9, Shaji Kunnathu Kumar10, Alli Murugesan11, Tony Reiman12, A. Keith Stewart2, Suzanne Trudel1, Trevor J. Pugh13

1Princess Margaret Cancer Centre and Department of Medical Biophysics, University of Toronto, Toronto, ON, Canada,2Princess Margaret Cancer Centre, Toronto, ON, Canada,3School of Integrated Health, University of New Brunswick, Saint John, NB, Canada,4Department of Biological Sciences, University of New Brunswick, Saint John, NB, Canada,5Sunnybrook Health Sciences Centre, Toronto, ON, Canada,6Dalhousie University and QEII Health Sciences Centre, Halifax, NS, Canada,7Cross Cancer Institute, Edmonton, AB, Canada,8Vancouver General Hospital, Vancouver, BC, Canada,9Mayo Clinic Arizona, Scottsdale, AZ,10Professor of Medicine, Dept. of Hematology, Mayo Clinic, Rochester, MN,11Faculty of Medicine, Dalhousie University, and Department of Nursing and Health Sciences, Faculty of Science, Applied Science and Engineering, University of New Brunswick, Saint John, NB, Canada,12Saint John Regional Hospital, Saint John, NB, Canada,13Princess Margaret Cancer Centre; Department of Medical Biophysics, University of Toronto, and Ontario Institute for Cancer Research, Toronto, ON, Canada

摘要 Abstract

Introduction: Early relapse limits durable remissions in multiple myeloma (MM). Cell-free DNA (cfDNA) fragment patterns capture tumor burden and nucleosome positioning. We tested whether a fragmentomics signature trained at MRD time points stratifies progression-free survival (PFS) when applied to pretreatment plasma. Methods: We performed 30-40× whole-genome sequencing of plasma cfDNA from 43 newly diagnosed MM patients, with 65 additional MRD timepoint samples from 41 of those patients (post-ASCT n=30; 1-year maintenance n=30; other maintenance n=5) across eight Canadian sites (TFRIM4 and IMMAGINE studies) and one U.S. site (Mayo SPORE). MRD testing used multiparameter flow cytometry for all follow-up samples (n=65) and clonoSEQ in a subset (n=31). Logistic and elastic-net models were trained at MRD timepoints on fragmentomics features (short-fragment burden; a combined model integrating fragment-length distributions with inferred nucleosome positioning at MM-specific chromatin accessibility regions [Ordoñez et al., Genome Res. 2020]). A decision threshold was fixed by the Youden index during training and applied unchanged to diagnosis samples. PFS was analyzed by Kaplan-Meier, log-rank, and Cox models. Results: After a median follow-up of 49.1 months, 16 of 43 patients (37%) progressed. Using the prespecified locked threshold, patients classified as MRD+ by the proportion-of-short-fragments model had significantly shorter PFS than MRD- patients (HR = 5.12; 95% CI 1.16-22.57; log-rank p = 0.016), with median PFS of 49.2 months for MRD+ cases versus not reached for the MRD- group. Fixed-horizon PFS favored MRD- samples at 24/36/48 months (100/94/87% vs 85/81/53% for MRD+). A combined model integrating weighted fragment lengths with inferred nucleosome positioning also separated outcomes (log-rank p=0.054); the Cox HR was not estimable because no MRD- patients relapsed. At 24, 36, and 48 months, baseline MRD positivity by the short-fragment model identified 100%, 83%, and 86% of patients who relapsed within those intervals (specificity 44%, 43%, and 52%), while the combined model detected all early relapses across the same horizons (specificity 15-21%), indicating consistently high sensitivity but modest specificity for predicting early progression. Conclusions: A cfDNA fragmentomics signature trained at MRD time points stratified PFS when applied to diagnostic plasma, identifying patients at risk of early relapse. Short-fragment burden was most discriminative, and a combined model with nucleosome positioning recapitulated it with higher sensitivity, albeit lower specificity. These data support cfDNA fragmentomics as a practical liquid-biopsy risk biomarker in MM and suggest higher signals may proxy aggressive disease with greater tumor shedding and chromatin disorganization. Future work will validate findings in larger cohorts and integrate cytogenetic and immune features.
利益披露 Disclosure
D. D. Abelman, None.. J. Eagles, None.. A. Wong, None.. S. Shah, None.. J. Bruce, None. S. Pedersen, University Health Network Patent. Dynacare Patent. D. S. Scott, None.. C. Bonolo de Campos, None.. S. Chow, None. D. White, Janssen Other, Honoraria. Novartis Other, Honoraria. Forus Therapeutics Other, Honoraria. Sanofi Other, Honoraria. Antengene Other, Honoraria. Pfizer Other, Honoraria. GlaxoSmithKline Other, Honoraria. I. Sandhu, None. K. Song, Novartis Other, Honoraria. Janssen Other, Honoraria. GlaxoSmithKline Other, Honoraria. Bristol Myers Squibb Other, Honoraria. Gilead Other, Honoraria. Sanofi Other, Honoraria. S. K. Kumar, CVS Caremark Independent Contractor. BD Biosciences Independent Contractor. AbbVie ), Other, Consulting with no personal compensation. Amgen ), Other, Consulting with no personal compensation. ArcellX Other, Consulting with no personal compensation. BeiGene Other, Consulting with no personal compensation. Bristol Myers Squibb ), Other, Consulting with no personal compensation. AstraZeneca ). Carsgen ), Other, Consulting with no personal compensation. GSK ), Other, Consulting with no personal compensation. Janssen ), Other, Consulting with no personal compensation. K36 Other, Consulting with no personal compensation. Moderna Other, Consulting with no personal compensation. Pfizer Other, Consulting with no personal compensation. Regeneron Other, Consulting with no personal compensation. Roche-Genentech ), Other, Consulting with no personal compensation. Sanofi ), Other, Consulting with no personal compensation. Takeda ), Other, Consulting with no personal compensation. Gracell Bio ). Oricell ). A. Murugesan, None.. T. Reiman, None.. A. Stewart, None. S. Trudel, Janssen ), Other, Honoraria. Pfizer ), Other, Honoraria. Kite Other, Honoraria. GlaxoSmithKline Independent Contractor, Other, Honoraria. Sanofi Other, Honoraria. Roche Independent Contractor, ), Other, Honoraria. K36 Therapeutics ), Other, Honoraria. Bristol Myers Squibb ). T. J. Pugh, Roche Independent Contractor, ). AstraZeneca Independent Contractor, ). Merck Independent Contractor. Chrysalis Biomedical Advisors Independent Contractor. Genentech ). University Health Network Patent. Dynacare Patent.

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