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Literature DB >> 30249784

Minimal residual disease negativity using deep sequencing is a major prognostic factor in multiple myeloma.

Aurore Perrot¹, Valerie Lauwers-Cances², Jill Corre^3,4, Nelly Robillard⁵, Cyrille Hulin⁶, Marie-Lorraine Chretien⁷, Thomas Dejoie⁸, Sabrina Maheo^3,4, Anne-Marie Stoppa⁹, Brigitte Pegourie¹⁰, Lionel Karlin¹¹, Laurent Garderet¹², Bertrand Arnulf¹³, Chantal Doyen¹⁴, Nathalie Meuleman¹⁵, Bruno Royer¹⁶, Jean-Richard Eveillard¹⁷, Lotfi Benboubker¹⁸, Mamoun Dib¹⁹, Olivier Decaux²⁰, Arnaud Jaccard²¹, Karim Belhadj²², Sabine Brechignac²³, Brigitte Kolb²⁴, Cecile Fohrer²⁵, Mohamad Mohty¹², Margaret Macro²⁶, Paul G Richardson²⁷, Victoria Carlton²⁸, Martin Moorhead²⁸, Tom Willis²⁸, Malek Faham²⁸, Kenneth C Anderson²⁷, Jean-Luc Harousseau²⁹, Xavier Leleu³⁰, Thierry Facon³¹, Philippe Moreau³², Michel Attal³³, Hervé Avet-Loiseau^3,4, Nikhil Munshi²⁷.

Abstract

The introduction of novel agents has led to major improvements in clinical outcomes for patients with multiple myeloma. To shorten evaluation times for new treatments, health agencies are currently examining minimal residual disease (MRD) as a surrogate end point in clinical trials. We assessed the prognostic value of MRD, measured during maintenance therapy by next-generation sequencing (NGS). MRD negativity was defined as the absence of tumor plasma cell within 1 000 000 bone marrow cells (<10-6). Data were analyzed from a recent clinical trial that evaluated the role of transplantation in newly diagnosed myeloma patients treated with lenalidomide, bortezomib, and dexamethasone (RVD). MRD negativity was achieved at least once during maintenance in 127 patients (25%). At the start of maintenance therapy, MRD was a strong prognostic factor for both progression-free survival (adjusted hazard ratio, 0.22; 95% confidence interval, 0.15-0.34; P < .001) and overall survival (adjusted hazard ratio, 0.24; 95% confidence interval, 0.11-0.54; P = .001). Patients who were MRD negative had a higher probability of prolonged progression-free survival than patients with detectable residual disease, regardless of treatment group (RVD vs transplant), cytogenetic risk profile, or International Staging System disease stage at diagnosis. These results were similar after completion of maintenance therapy. Our findings confirm the value of MRD status, as determined by NGS, as a prognostic biomarker in multiple myeloma, and suggest that this approach could be used to adapt treatment strategies in future clinical trials.

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Year: 2018 PMID： 30249784 PMCID： PMC6284215 DOI： 10.1182/blood-2018-06-858613

Source DB: PubMed Journal: Blood ISSN： 0006-4971 Impact factor: 25.476

22 in total

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92 in total

1. Daratumumab, lenalidomide, bortezomib, and dexamethasone for transplant-eligible newly diagnosed multiple myeloma: the GRIFFIN trial.

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Journal: Best Pract Res Clin Haematol Date: 2020-01-17 Impact factor: 3.020

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Journal: Blood Date: 2019-11-28 Impact factor: 22.113

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Journal: Br J Haematol Date: 2020-02-05 Impact factor: 6.998

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Authors: Surbhi Sidana; Eli Muchtar; M Hasib Sidiqi; Dragan Jevremovic; Angela Dispenzieri; Wilson Gonsalves; Francis Buadi; Martha Q Lacy; Suzanne R Hayman; Taxiarchis Kourelis; Prashant Kapoor; Ronald S Go; Rahma Warsame; Nelson Leung; S Vincent Rajkumar; Robert A Kyle; Morie A Gertz; Shaji K Kumar
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Authors: Jagoda K Jasielec; Tadeusz Kubicki; Noopur Raje; Ravi Vij; Donna Reece; Jesus Berdeja; Benjamin A Derman; Cara A Rosenbaum; Paul Richardson; Sandeep Gurbuxani; Sarah Major; Brittany Wolfe; Andrew T Stefka; Leonor Stephens; Kathryn M Tinari; Tyler Hycner; Alexandra E Rojek; Dominik Dytfeld; Kent A Griffith; Todd M Zimmerman; Andrzej J Jakubowiak
Journal: Blood Date: 2020-11-26 Impact factor: 22.113