| Literature DB >> 21339757 |
P A Greif1, S H Eck, N P Konstandin, A Benet-Pagès, B Ksienzyk, A Dufour, A T Vetter, H D Popp, B Lorenz-Depiereux, T Meitinger, S K Bohlander, T M Strom.
Abstract
Genetic lesions are crucial for cancer initiation. Recently, whole genome sequencing, using next generation technology, was used as a systematic approach to identify mutations in genomes of various types of tumors including melanoma, lung and breast cancer, as well as acute myeloid leukemia (AML). Here, we identify tumor-specific somatic mutations by sequencing transcriptionally active genes. Mutations were detected by comparing the transcriptome sequence of an AML sample with the corresponding remission sample. Using this approach, we found five non-synonymous mutations specific to the tumor sample. They include a nonsense mutation affecting the RUNX1 gene, which is a known mutational target in AML, and a missense mutation in the putative tumor suppressor gene TLE4, which encodes a RUNX1 interacting protein. Another missense mutation was identified in SHKBP1, which acts downstream of FLT3, a receptor tyrosine kinase mutated in about 30% of AML cases. The frequency of mutations in TLE4 and SHKBP1 in 95 cytogenetically normal AML patients was 2%. Our study demonstrates that whole transcriptome sequencing leads to the rapid detection of recurring point mutations in the coding regions of genes relevant to malignant transformation.Entities:
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Year: 2011 PMID: 21339757 DOI: 10.1038/leu.2011.19
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528