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Whole tumor analysis reveals early origin of the TERT promoter mutation and intercellular heterogeneity in TERT expression

PDGFRA公司 桑格测序 生物 癌症研究 放大器 分子生物学 IDH1 少突胶质瘤 突变体 肿瘤进展 突变 胶质瘤 脑瘤 癌基因 野生型 癌症 基因 聚合酶链反应 细胞周期 遗传学 星形细胞瘤 病理 医学 间质细胞 主旨
作者
Christina Appin,Chibo Hong,Abigail Suwala,Stephanie Hilz,Radhika Mathur,David A. Solomon,Ivan Smirnov,Nicholas Stevers,Anny Shai,Albert Wang,Mitchel S. Berger,Susan M. Chang,Joanna J. Phillips,J Costello
出处
期刊:Neuro-oncology [Oxford University Press]
卷期号:26 (4): 640-652 被引量:4
标识
DOI:10.1093/neuonc/noad231
摘要

Abstract Background The TERT promoter mutation (TPM) is acquired in most IDH-wildtype glioblastomas (GBM) and IDH-mutant oligodendrogliomas (OD) enabling tumor cell immortality. Previous studies on TPM clonality show conflicting results. This study was performed to determine whether TPM is clonal on a tumor-wide scale. Methods We investigated TPM clonality in relation to presumed early events in 19 IDH-wildtype GBM and 10 IDH-mutant OD using 3-dimensional comprehensive tumor sampling. We performed Sanger sequencing on 264 tumor samples and deep amplicon sequencing on 187 tumor samples. We obtained tumor purity and copy number estimates from whole exome sequencing. TERT expression was assessed by RNA-seq and RNAscope. Results We detected TPM in 100% of tumor samples with quantifiable tumor purity (219 samples). Variant allele frequencies (VAF) of TPM correlate positively with chromosome 10 loss in GBM (R = 0.85), IDH1 mutation in OD (R = 0.87), and with tumor purity (R = 0.91 for GBM; R = 0.90 for OD). In comparison, oncogene amplification was tumor-wide for MDM4- and most EGFR-amplified cases but heterogeneous for MYCN and PDGFRA, and strikingly high in low-purity samples. TPM VAF was moderately correlated with TERT expression (R = 0.52 for GBM; R = 0.65 for OD). TERT expression was detected in a subset of cells, solely in TPM-positive samples, including samples equivocal for tumor. Conclusions On a tumor-wide scale, TPM is among the earliest events in glioma evolution. Intercellular heterogeneity of TERT expression, however, suggests dynamic regulation during tumor growth. TERT expression may be a tumor cell-specific biomarker.

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