A molecular compendium of genes expressed in multiple myeloma

Author:

Claudio Jaime O.1,Masih-Khan Esther1,Tang Hongchang1,Gonçalves Jason1,Voralia Michael1,Li Zhi Hua1,Nadeem Vincent1,Cukerman Eva1,Francisco-Pabalan Ofelia1,Liew Choong Chin1,Woodgett James R.1,Stewart A. Keith1

Affiliation:

1. From the Division of Experimental Therapeutics, Toronto General Research Institute, and from Ontario Cancer Institute, University Health Network; both of Toronto, ON; and the Cardiovascular Genome Unit, Brigham and Women's Hospital, Harvard Medical School, Boston, MA.

Abstract

Abstract We have created a molecular resource of genes expressed in primary malignant plasma cells using a combination of cDNA library construction, 5′ end single-pass sequencing, bioinformatics, and microarray analysis. In total, we identified 9732 nonredundant expressed genes. This dataset is available as the Myeloma Gene Index (www.uhnres.utoronto.ca/akstewart_lab).Predictably, the sequenced profile of myeloma cDNAs mirrored the known function of immunoglobulin-producing, high-respiratory rate, low-cycling, terminally differentiated plasma cells. Nevertheless, approximately 10% of myeloma-expressed sequences matched only entries in the database of Expressed Sequence Tags (dbEST) or the high-throughput genomic sequence (htgs) database. Numerous novel genes of potential biologic significance were identified. We therefore spotted 4300 sequenced cDNAs on glass slides creating a myeloma-enriched microarray. Several of the most highly expressed genes identified by sequencing, such as a novel putative disulfide isomerase (MGC3178), tumor rejection antigen TRA1, heat shock 70-kDa protein 5, and annexin A2, were also differentially expressed between myeloma and B lymphoma cell lines using this myeloma-enriched microarray. Furthermore, a defined subset of 34 up-regulated and 18 down-regulated genes on the array were able to differentiate myeloma from nonmyeloma cell lines. These not only include genes involved in B-cell biology such as syndecan, BCMA, PIM2, MUM1/IRF4,and XBP1, but also novel uncharacterized genes matching sequences only in the public databases. In summary, our expressed gene catalog and myeloma-enriched microarray contains numerous genes of unknown function and may complement other commercially available arrays in defining the molecular portrait of this hematopoietic malignancy.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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