Genome-Wide Somatic Alterations in Multiple Myeloma Reveal a Superior Outcome Group

Genome-Wide Somatic Alterations in Multiple Myeloma Reveal a Superior Outcome Group

Multiple myeloma (MM) is accompanied by heterogeneous somatic alterations. The overall goal of this study was to describe the genomic landscape of myeloma using deep whole-genome sequencing (WGS) and develop a model that identifies patients with long survival. We analyzed deep WGS data from 183 newl...

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Veröffentlicht in:Journal of clinical oncology 2020-09, Vol.38 (27), p.3107-3118
Hauptverfasser: Samur, Mehmet Kemal, Aktas Samur, Anil, Fulciniti, Mariateresa, Szalat, Raphael, Han, Tessa, Shammas, Masood, Richardson, Paul, Magrangeas, Florence, Minvielle, Stephane, Corre, Jill, Moreau, Philippe, Thakurta, Anjan, Anderson, Kenneth C, Parmigiani, Giovanni, Avet-Loiseau, Hervé, Munshi, Nikhil C
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Aged
Antineoplastic Combined Chemotherapy Protocols - therapeutic use
Biomarkers, Tumor - genetics
Bortezomib - administration & dosage
Cancer
Combined Modality Therapy
Dexamethasone
DNA Mutational Analysis
DNA, Neoplasm
Female
GTP Phosphohydrolases - genetics
Humans
INDEL Mutation
Lenalidomide - administration & dosage
Life Sciences
Male
Membrane Proteins - genetics
Middle Aged
Multiple Myeloma - genetics
Multiple Myeloma - therapy
ORIGINAL REPORTS
Progression-Free Survival
Stem Cell Transplantation
Survival Rate
Treatment Outcome
Whole Genome Sequencing
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Zusammenfassung:Multiple myeloma (MM) is accompanied by heterogeneous somatic alterations. The overall goal of this study was to describe the genomic landscape of myeloma using deep whole-genome sequencing (WGS) and develop a model that identifies patients with long survival. We analyzed deep WGS data from 183 newly diagnosed patients with MM treated with lenalidomide, bortezomib, and dexamethasone (RVD) alone or RVD + autologous stem cell transplant (ASCT) in the IFM/DFCI 2009 study (ClinicalTrials.gov identifier: NCT01191060). We integrated genomic markers with clinical data. We report significant variability in mutational load and processes within MM subgroups. The timeline of observed activation of mutational processes provides the basis for 2 distinct models of acquisition of mutational changes detected at the time of diagnosis of myeloma. Virtually all MM subgroups have activated DNA repair-associated signature as a prominent late mutational process, whereas APOBEC signature targeting C>G is activated in the intermediate phase of disease progression in high-risk MM. Importantly, we identify a genomically defined MM subgroup (17% of newly diagnosed patients) with low DNA damage (low genomic scar score with chromosome 9 gain) and a superior outcome (100% overall survival at 69 months), which was validated in a large independent cohort. This subgroup allowed us to distinguish patients with low- and high-risk hyperdiploid MM and identify patients with prolongation of progression-free survival. Genomic characteristics of this subgroup included lower mutational load with significant contribution from age-related mutations as well as frequent mutation. Surprisingly, their overall survival was independent of International Staging System and minimal residual disease status. This is a comprehensive study identifying genomic markers of a good-risk group with prolonged survival. Identification of this patient subgroup will affect future therapeutic algorithms and research planning.
ISSN:0732-183X
1527-7755
1527-7755
DOI:10.1200/jco.20.00461