| Literature DB >> 29616851 |
Hogune Im1, Varsha Rao1, Kunju Sridhar2, Jason Bentley3, Tejaswini Mishra1, Rui Chen1, Jeff Hall4, Armin Graber4, Yan Zhang5, Xiao Li5, George I Mias6, Michael P Snyder1, Peter L Greenberg2.
Abstract
To provide biologic insights into mechanisms underlying myelodysplastic syndromes (MDS) we evaluated the CD34+ marrow cells transcriptome using high-throughput RNA sequencing (RNA-Seq). We demonstrated significant differential gene expression profiles (GEPs) between MDS and normal and identified 41 disease classifier genes. Additionally, two main clusters of GEPs distinguished patients based on their major clinical features, particularly between those whose disease remained stable versus patients who transformed into acute myeloid leukemia within 12 months. The genes whose expression was associated with disease outcome were involved in functional pathways and biologic processes highly relevant for MDS. Combined with exomic analysis we identified differential isoform usage of genes in MDS mutational subgroups, with consequent dysregulation of distinct biologic functions. This combination of clinical, transcriptomic and exomic findings provides valuable understanding of mechanisms underlying MDS and its progression to a more aggressive stage and also facilitates prognostic characterization of MDS patients.Entities:
Keywords: Myeloid leukemias and dysplasias; isoform usage; myeloproliferative disorders; trancriptomics
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Year: 2018 PMID: 29616851 PMCID: PMC6214785 DOI: 10.1080/10428194.2018.1452210
Source DB: PubMed Journal: Leuk Lymphoma ISSN: 1026-8022