Autor: |
de Rooij, Jasmijn D E, Branstetter, Cristyn, Ma, Jing, Li, Yongjin, Walsh, Michael P, Cheng, Jinjun, Obulkasim, Askar, Dang, Jinjun, Easton, John, Verboon, Lonneke J, Mulder, Heather L, Zimmermann, Martin, Koss, Cary, Gupta, Pankaj, Edmonson, Michael, Rusch, Michael, Lim, Joshua Yew Suang, Reinhardt, Katarina, Pigazzi, Martina, Song, Guangchun, Yeoh, Allen Eng Juh, Shih, Lee-Yung, Liang, Der-Cherng, Halene, Stephanie, Krause, Diane S, Zhang, Jinghui, Downing, James R, Locatelli, Franco, Reinhardt, Dirk, van den Heuvel-Eibrink, Marry M, Zwaan, C Michel, Fornerod, Maarten, Gruber, Tanja A |
Zdroj: |
Nature Genetics; March 2017, Vol. 49 Issue: 3 p451-456, 6p |
Abstrakt: |
Acute megakaryoblastic leukemia (AMKL) is a subtype of acute myeloid leukemia (AML) in which cells morphologically resemble abnormal megakaryoblasts. While rare in adults, AMKL accounts for 4–15% of newly diagnosed childhood AML cases. AMKL in individuals without Down syndrome (non-DS-AMKL) is frequently associated with poor clinical outcomes. Previous efforts have identified chimeric oncogenes in a substantial number of non-DS-AMKL cases, including RBM15-MKL1, CBFA2T3-GLIS2, KMT2A gene rearrangements, and NUP98-KDM5A. However, the etiology of 30–40% of cases remains unknown. To better understand the genomic landscape of non-DS-AMKL, we performed RNA and exome sequencing on specimens from 99 patients (75 pediatric and 24 adult). We demonstrate that pediatric non-DS-AMKL is a heterogeneous malignancy that can be divided into seven subgroups with varying outcomes. These subgroups are characterized by chimeric oncogenes with cooperating mutations in epigenetic and kinase signaling genes. Overall, these data shed light on the etiology of AMKL and provide useful information for the tailoring of treatment. |
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