Clonal competition with alternating dominance in multiple myeloma

Author:

Keats Jonathan J.1,Chesi Marta1,Egan Jan B.1,Garbitt Victoria M.1,Palmer Stephen E.1,Braggio Esteban1,Van Wier Scott1,Blackburn Patrick R.1,Baker Angela S.2,Dispenzieri Angela3,Kumar Shaji3,Rajkumar S. Vincent3,Carpten John D.2,Barrett Michael2,Fonseca Rafael1,Stewart A. Keith1,Bergsagel P. Leif1

Affiliation:

1. Comprehensive Cancer Center, Mayo Clinic Arizona, Scottsdale, AZ;

2. Translational Genomics Research Institute, Phoenix, AZ; and

3. Division of Hematology, Mayo Clinic, Rochester, MN

Abstract

Abstract Emerging evidence indicates that tumors can follow several evolutionary paths over a patient's disease course. With the use of serial genomic analysis of samples collected at different points during the disease course of 28 patients with multiple myeloma, we found that the genomes of standard-risk patients show few changes over time, whereas those of cytogenetically high-risk patients show significantly more changes over time. The results indicate the existence of 3 temporal tumor types, which can either be genetically stable, linearly evolving, or heterogeneous clonal mixtures with shifting predominant clones. A detailed analysis of one high-risk patient sampled at 7 time points over the entire disease course identified 2 competing subclones that alternate in a back and forth manner for dominance with therapy until one clone underwent a dramatic linear evolution. With the use of the Vk*MYC genetically engineered mouse model of myeloma we modeled this competition between subclones for predominance occurring spontaneously and with therapeutic selection.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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