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Title: Gene expression profiling for molecular classification of multiple myeloma in newly diagnosed patients.
Author(s): Broyl, A.
Hose, D.
Lokhorst, H.
Knegt, Y. de
Peeters, J.
Jauch, A.
Bertsch, U.
Buijs, A.
Stevens-Kroef, M.J.P.L. (298204789)
Beverloo, H.B.
Vellenga, E.
Zweegman, S.
Kersten, M.J.
Holt, B. van der
Jarari, L. el
Mulligan, G.
Goldschmidt, H.
Duin, M. van
Sonneveld, P.
Publication year: 2010
Document type: Article / Letter to editor
Journal: Blood
ISSN: 0006-4971
Volume: vol. 116
Issue: iss. 14
Start page: p. 2543
End page: p. 2553
Abstract: To identify molecularly defined subgroups in multiple myeloma, gene expression profiling was performed on purified CD138(+) plasma cells of 320 newly diagnosed myeloma patients included in the Dutch-Belgian/German HOVON-65/GMMG-HD4 trial. Hierarchical clustering identified 10 subgroups; 6 corresponded to clusters described in the University of Arkansas for Medical Science (UAMS) classification, CD-1 (n = 13, 4.1%), CD-2 (n = 34, 1.6%), MF (n = 32, 1.0%), MS (n = 33, 1.3%), proliferation-associated genes (n = 15, 4.7%), and hyperdiploid (n = 77, 24.1%). Moreover, the UAMS low percentage of bone disease cluster was identified as a subcluster of the MF cluster (n = 15, 4.7%). One subgroup (n = 39, 12.2%) showed a myeloid signature. Three novel subgroups were defined, including a subgroup of 37 patients (11.6%) characterized by high expression of genes involved in the nuclear factor kappa light-chain-enhancer of activated B cells pathway, which include TNFAIP3 and CD40. Another subgroup of 22 patients (6.9%) was characterized by distinct overexpression of cancer testis antigens without overexpression of proliferation genes. The third novel cluster of 9 patients (2.8%) showed up-regulation of protein tyrosine phosphatases PRL-3 and PTPRZ1 as well as SOCS3. To conclude, in addition to 7 clusters described in the UAMS classification, we identified 3 novel subsets of multiple myeloma that may represent unique diagnostic entities.
Subject: ONCOL 1: Hereditary cancer and cancer-related syndromes
Organization: UMCN Extern
Human Genetics
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/88517

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