Li Zhenli, Chen Geng, Cai Zhixiong, Dong Xiuqing, He Lei, Qiu Liman, Zeng Yongyi, Liu Xiaolong, Liu Jingfeng
The United Innovation of Mengchao Hepatobiliary Technology Key Laboratory of Fujian Province, Mengchao Hepatobiliary Hospital of Fujian Medical University, Fuzhou 350025, China.
Mengchao Med-X Center, Fuzhou University, Fuzhou 350116, China.
Chin J Cancer Res. 2021 Jun 30;33(3):364-378. doi: 10.21147/j.issn.1000-9604.2021.03.08.
Neoantigens derived from tumor-specific genomic alterations have demonstrated great potential for immunotherapeutic interventions in cancers. However, the comprehensive profile of hepatocellular carcinoma (HCC) neoantigens and their complex interplay with immune microenvironment and tumor evolution have not been fully addressed.
Here we integrated whole exome sequencing data, transcriptome sequencing data and clinical information of 72 primary HCC patients to characterize the HCC neoantigen profile, and systematically explored its interactions with tumor clonal evolution, driver mutations and immune microenvironments.
We observed that higher somatic mutation/neoantigen load was associated with better clinical outcomes and HCC patients could be further divided into two subgroups with distinct prognosis based on their neoantigen expression patterns. HCC subgroup with neoantigen expression probability high (NEP-H) showed more aggressive pathologic features including increased incidence of tumor thrombus (P=0.038), higher recurrence rate (P=0.029), more inclined to lack tumor capsule (P=0.026) and with more microsatellite instability sites (P=0.006). In addition, NEP-H subgroup was also characterized by higher chance to be involved in tumor clonal evolution [odds ratio (OR)=46.7, P<0.001]. Gene set enrichment analysis revealed that upregulation of MYC and its targets could suppress immune responses, leading to elevated neoantigen expression proportion in tumor cells. Furthermore, we discovered an immune escape mechanism that tumors could become more inconspicuous by evolving subclones with less immunogenicity. We observed that smaller clonal mutation clusters with higher immunogenicity in tumor were more likely to involve in clonal evolution. Based on identified neoantigen profiles, we also discovered series of neoantigenic hotspot genes, which could serve as potential actionable targets in future.
Our results revealed the landscape of HCC neoantigens and discovered two clinically relevant subgroups with distinct neoantigen expression patterns, suggesting the neoantigen expression should be fully considered in future immunotherapeutic interventions.
源自肿瘤特异性基因组改变的新抗原已在癌症免疫治疗干预中展现出巨大潜力。然而,肝细胞癌(HCC)新抗原的全面概况及其与免疫微环境和肿瘤进化的复杂相互作用尚未得到充分研究。
在此,我们整合了72例原发性HCC患者的全外显子组测序数据、转录组测序数据和临床信息,以表征HCC新抗原概况,并系统地探究其与肿瘤克隆进化、驱动突变和免疫微环境的相互作用。
我们观察到较高的体细胞突变/新抗原负荷与更好的临床结果相关,并且HCC患者可根据其新抗原表达模式进一步分为两个预后不同的亚组。新抗原表达概率高(NEP-H)的HCC亚组表现出更具侵袭性的病理特征,包括肿瘤血栓发生率增加(P = 0.038)、更高的复发率(P = 0.029)、更倾向于缺乏肿瘤包膜(P = 0.026)以及更多的微卫星不稳定性位点(P = 0.006)。此外,NEP-H亚组还具有更高的参与肿瘤克隆进化的几率[优势比(OR)= 46.7,P < 0.001]。基因集富集分析表明,MYC及其靶标的上调可抑制免疫反应,导致肿瘤细胞中新抗原表达比例升高。此外,我们发现了一种免疫逃逸机制,即肿瘤可通过进化出免疫原性较低的亚克隆而变得更不明显。我们观察到肿瘤中具有较高免疫原性的较小克隆突变簇更有可能参与克隆进化。基于鉴定出的新抗原概况,我们还发现了一系列新抗原热点基因,它们可能成为未来潜在的可操作靶点。
我们的结果揭示了HCC新抗原的全貌,并发现了两个具有不同新抗原表达模式的临床相关亚组,表明在未来的免疫治疗干预中应充分考虑新抗原表达。
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