Genomic sequencing of meningiomas identifies oncogenic SMO and AKT1 mutations
Jones, Robert T.
Van Hummelen, Paul
Ducar, Matthew D.
MacConaill, Laura E.
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CitationBrastianos, P. K., P. M. Horowitz, S. Santagata, R. T. Jones, A. McKenna, G. Getz, K. L. Ligon, et al. 2013. “Genomic sequencing of meningiomas identifies oncogenic SMO and AKT1 mutations.” Nature genetics 45 (3): 285-289. doi:10.1038/ng.2526. http://dx.doi.org/10.1038/ng.2526.
AbstractMeningiomas are the most common primary nervous system tumor. The tumor suppressor NF2 is disrupted in approximately half of meningiomas1 but the complete spectrum of genetic changes remains undefined. We performed whole-genome or whole-exome sequencing on 17 meningiomas and focused sequencing on an additional 48 tumors to identify and validate somatic genetic alterations. Most meningiomas exhibited simple genomes, with fewer mutations, rearrangements, and copy-number alterations than reported in other adult tumors. However, several meningiomas harbored more complex patterns of copy-number changes and rearrangements including one tumor with chromothripsis. We confirmed focal NF2 inactivation in 43% of tumors and found alterations in epigenetic modifiers among an additional 8% of tumors. A subset of meningiomas lacking NF2 alterations harbored recurrent oncogenic mutations in AKT1 (E17K) and SMO (W535L) and exhibited immunohistochemical evidence of activation of their pathways. These mutations were present in therapeutically challenging tumors of the skull base and higher grade. These results begin to define the spectrum of genetic alterations in meningiomas and identify potential therapeutic targets.
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