| Literature DB >> 28892075 |
Yosef E Maruvka1,2, Kent W Mouw3,4, Rosa Karlic5, Prasanna Parasuraman1, Atanas Kamburov1,2, Paz Polak1,2, Nicholas J Haradhvala1,2, Julian M Hess2, Esther Rheinbay1,2, Yehuda Brody2, Amnon Koren6, Lior Z Braunstein1,2, Alan D'Andrea2,3,4, Michael S Lawrence1,2, Adam Bass2,7, Andre Bernards1, Franziska Michor2,3,8,9, Gad Getz1,2,3,10.
Abstract
Microsatellites (MSs) are tracts of variable-length repeats of short DNA motifs that exhibit high rates of mutation in the form of insertions or deletions (indels) of the repeated motif. Despite their prevalence, the contribution of somatic MS indels to cancer has been largely unexplored, owing to difficulties in detecting them in short-read sequencing data. Here we present two tools: MSMuTect, for accurate detection of somatic MS indels, and MSMutSig, for identification of genes containing MS indels at a higher frequency than expected by chance. Applying MSMuTect to whole-exome data from 6,747 human tumors representing 20 tumor types, we identified >1,000 previously undescribed MS indels in cancer genes. Additionally, we demonstrate that the number and pattern of MS indels can accurately distinguish microsatellite-stable tumors from tumors with microsatellite instability, thus potentially improving classification of clinically relevant subgroups. Finally, we identified seven MS indel driver hotspots: four in known cancer genes (ACVR2A, RNF43, JAK1, and MSH3) and three in genes not previously implicated as cancer drivers (ESRP1, PRDM2, and DOCK3).Entities:
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Year: 2017 PMID: 28892075 PMCID: PMC9123850 DOI: 10.1038/nbt.3966
Source DB: PubMed Journal: Nat Biotechnol ISSN: 1087-0156 Impact factor: 68.164