Accelerated single cell seeding in relapsed multiple myeloma

Author:

Landau Heather J.,Yellapantula Venkata,Diamond Benjamin T.,Rustad Even H.ORCID,Maclachlan Kylee H.,Gundem Gunes,Medina-Martinez Juan,Ossa Juan Arango,Levine Max F.ORCID,Zhou Yangyu,Kappagantula Rajya,Baez Priscilla,Attiyeh MarcORCID,Makohon-Moore Alvin,Zhang Lance,Boyle Eileen M.,Ashby CodyORCID,Blaney Patrick,Patel Minal,Zhang Yanming,Dogan AhmetORCID,Chung David J.,Giralt Sergio,Lahoud Oscar B.,Peled Jonathan U.,Scordo Michael,Shah Gunjan,Hassoun Hani,Korde Neha S.,Lesokhin Alexander M.,Lu Sydney,Mailankody Sham,Shah UrviORCID,Smith Eric,Hultcrantz Malin L.ORCID,Ulaner Gary A.,van Rhee Frits,Morgan Gareth J.,Landgren OlaORCID,Papaemmanuil ElliORCID,Iacobuzio-Donahue ChristineORCID,Maura FrancescoORCID

Abstract

AbstractMultiple myeloma (MM) progression is characterized by the seeding of cancer cells in different anatomic sites. To characterize this evolutionary process, we interrogated, by whole genome sequencing, 25 samples collected at autopsy from 4 patients with relapsed MM and an additional set of 125 whole exomes collected from 51 patients. Mutational signatures analysis showed how cytotoxic agents introduce hundreds of unique mutations in each surviving cancer cell, detectable by bulk sequencing only in cases of clonal expansion of a single cancer cell bearing the mutational signature. Thus, a unique, single-cell genomic barcode can link chemotherapy exposure to a discrete time window in a patient′s life. We leveraged this concept to show that MM systemic seeding is accelerated at relapse and appears to be driven by the survival and subsequent expansion of a single myeloma cell following treatment with high-dose melphalan therapy and autologous stem cell transplant.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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