Clinical drug resistance linked to interconvertible phenotypic and functional states of tumor-propagating cells in multiple myeloma.

نویسندگان

  • Aristeidis Chaidos
  • Chris P Barnes
  • Gillian Cowan
  • Philippa C May
  • Valeria Melo
  • Evdoxia Hatjiharissi
  • Maria Papaioannou
  • Heather Harrington
  • Helen Doolittle
  • Evangelos Terpos
  • Meletios Dimopoulos
  • Saad Abdalla
  • Helen Yarranton
  • Kikkeri Naresh
  • Letizia Foroni
  • Alistair Reid
  • Amin Rahemtulla
  • Michael Stumpf
  • Irene Roberts
  • Anastasios Karadimitris
چکیده

The phenotype and function of cells enriched in tumor-propagating activity and their relationship to the phenotypic architecture in multiple myeloma (MM) are controversial. Here, in a cohort of 30 patients, we show that MM composes 4 hierarchically organized, clonally related subpopulations, which, although phenotypically distinct, share the same oncogenic chromosomal abnormalities as well as immunoglobulin heavy chain complementarity region 3 area sequence. Assessed in xenograft assays, myeloma-propagating activity is the exclusive property of a population characterized by its ability for bidirectional transition between the dominant CD19(-)CD138(+) plasma cell (PC) and a low frequency CD19(-)CD138(-) subpopulation (termed Pre-PC); in addition, Pre-PCs are more quiescent and unlike PCs, are primarily localized at extramedullary sites. As shown by gene expression profiling, compared with PCs, Pre-PCs are enriched in epigenetic regulators, suggesting that epigenetic plasticity underpins the phenotypic diversification of myeloma-propagating cells. Prospective assessment in paired, pretreatment, and posttreatment bone marrow samples shows that Pre-PCs are up to 300-fold more drug-resistant than PCs. Thus, clinical drug resistance in MM is linked to reversible, bidirectional phenotypic transition of myeloma-propagating cells. These novel biologic insights have important clinical implications in relation to assessment of minimal residual disease and development of alternative therapeutic strategies in MM.

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عنوان ژورنال:
  • Blood

دوره 121 2  شماره 

صفحات  -

تاریخ انتشار 2013