| Literature DB >> 28493366 |
Snjezana Dogan1, Deborah J Chute2, Bin Xu3, Ryan N Ptashkin1, Raghu Chandramohan1, Jacklyn Casanova-Murphy1, Khedoudja Nafa1, Justin A Bishop4, Simion I Chiosea5, Edward B Stelow6, Ian Ganly7, David G Pfister8, Nora Katabi1, Ronald A Ghossein1, Michael F Berger1,9.
Abstract
Sinonasal undifferentiated carcinoma (SNUC) is a high-grade malignancy with limited treatment options and poor outcome. A morphological spectrum of 47 sinonasal tumours including 17 (36.2%) SNUCs was analysed at genomic level. Thirty carcinomas (cohort 1) were subjected to a hybridization exon-capture next-generation sequencing assay (MSK-IMPACTTM ) to interrogate somatic variants in 279 or 410 cancer-related genes. Seventeen sinonasal tumours (cohort 2) were examined only for the presence of IDH1/2 exon 4 mutations by Sanger sequencing. IDH2 R172 single nucleotide variants were overall detected in 14 (82.4%) SNUCs, in two (20%) poorly-differentiated carcinomas with glandular/acinar differentiation, and in one of two high-grade neuroendocrine carcinomas, large cell type (HGNECs). No IDH2 mutation was detected in any of five olfactory neuroblastomas or in any of five SMARCB1-deficient carcinomas. Among 12 IDH2-mutated cases in cohort 1, five (41.7%) harboured co-existing TP53 mutations, four (33.3%) CDKN2A/2B loss-of-function alterations, four (33.3%) MYC amplification, and three (25%) had concurrent SETD2 mutations. AKT1 E17K and KIT D816V hotspot variants were each detected in one IDH2-mutated SNUC. The vast majority of SNUCs and variable proportions of other poorly-differentiated sinonasal carcinomas may be amenable to IDH2-targeted therapy.Entities:
Keywords: IDH2 R172; SNUC; sinonasal undifferentiated carcinoma
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Year: 2017 PMID: 28493366 PMCID: PMC5639875 DOI: 10.1002/path.4915
Source DB: PubMed Journal: J Pathol ISSN: 0022-3417 Impact factor: 9.883