Circumventing intratumoral heterogeneity to identify potential therapeutic targets in hepatocellular carcinoma

肝细胞癌 遗传异质性 外显子组测序 医学 六氯环己烷 肿瘤异质性 突变 生物 癌症研究 内科学 遗传学 基因 癌症 表型
作者
Ao Huang,Xin Zhao,Xin‐Rong Yang,Fuqiang Li,Xinlan Zhou,Kui Wu,Xin Zhang,Qi‐Man Sun,Ya Cao,Hongmei Zhu,Xiangdong Wang,Huanming Yang,Jian Wang,Zhao‐You Tang,Yong Hou,Jia Fan,Jian Zhou
出处
期刊:Journal of Hepatology [Elsevier BV]
卷期号:67 (2): 293-301 被引量:97
标识
DOI:10.1016/j.jhep.2017.03.005
摘要

Identifying target genetic mutations in hepatocellular carcinoma (HCC) for therapy is made challenging by intratumoral heterogeneity. Circulating cell-free DNAs (cfDNA) may contain a more complete mutational spectrum compared to a single tumor sample. This study aimed to identify the most efficient strategy to identify all the mutations within heterogeneous HCCs.Whole exome sequencing (WES) and targeted deep sequencing (TDS) were carried out in 32 multi-regional tumor samples from five patients. Matched preoperative cfDNAs were sequenced accordingly. Intratumoral heterogeneity was measured using the average percentage of non-ubiquitous mutations (present in parts of tumor regions). Profiling efficiencies of single tumor specimen and cfDNA were compared. The strategy with the highest performance was used to screen for actionable mutations.Variable levels of heterogeneity with branched and parallel evolution patterns were observed. The heterogeneity decreased at higher sequencing depth of TDS compared to measurements by WES (28.1% vs. 34.9%, p<0.01) but remained unchanged when additional samples were analyzed. TDS of single tumor specimen identified an average of 70% of the total mutations from multi-regional tissues. Although genome profiling efficiency of cfDNA increased with sequencing depth, an average of 47.2% total mutations were identified using TDS, suggesting that tissue samples outperformed it. TDS of single tumor specimen in 66 patients and cfDNAs in four unresectable HCCs showed that 38.6% (26/66 and 1/4) of patients carried mutations that were potential therapeutic targets.TDS of single tumor specimen could identify actionable mutations targets for therapy in HCC. cfDNA may serve as secondary alternative in profiling HCC genome.Targeted deep sequencing of single tumor specimen is a more efficient method to identify mutations in hepatocellular carcinoma made from mixed subtypes compared to circulating cell-free DNA in blood. cfDNA may serve as secondary alternative in profiling HCC genome. Identifying mutations may help clinicians choose targeted therapy for better individual treatments.
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