| Literature DB >> 32555163 |
Carolina Schinke1, Eileen M Boyle2, Cody Ashby2, Yan Wang2, Valeriy Lyzogubov2, Christopher Wardell2, Pingping Qu3, Antje Hoering3, Shayu Deshpande2, Katie Ryan2, Sharmilan Thanendrarajan2, Meera Mohan2, Naveen Yarlagadda2, Maliha Khan2, Samrat Roy Choudhury2, Maurizio Zangari2, Frits van Rhee2, Faith Davies2, Bart Barlogie4, Gareth Morgan2, Brian A Walker5,6.
Abstract
Primary plasma cell leukemia (pPCL) is a rare and aggressive form of multiple myeloma (MM) that is characterized by the presence of ≥20% circulating plasma cells. Overall survival remains poor despite advances of anti-MM therapy. The disease biology as well as molecular mechanisms that distinguish pPCL from non-pPCL MM remain poorly understood and, given the rarity of the disease, are challenging to study. In an attempt to identify key biological mechanisms that result in the aggressive pPCL phenotype, we performed whole-exome sequencing and gene expression analysis in 23 and 41 patients with newly diagnosed pPCL, respectively. The results reveal an enrichment of complex structural changes and high-risk mutational patterns in pPCL that explain, at least in part, the aggressive nature of the disease. In particular, pPCL patients with traditional low-risk features such as translocation t(11;14) or hyperdiploidy accumulated adverse risk genetic events that could account for the poor outcome in this group. Furthermore, gene expression profiling showed upregulation of adverse risk modifiers in pPCL compared to non-pPCL MM, while adhesion molecules and extracellular matrix proteins became increasingly downregulated. In conclusion, this is one of the largest studies to dissect pPCL on a genomic and molecular level.Entities:
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Year: 2020 PMID: 32555163 PMCID: PMC7303180 DOI: 10.1038/s41408-020-0336-z
Source DB: PubMed Journal: Blood Cancer J ISSN: 2044-5385 Impact factor: 11.037