Abstract 363: Investigating the potential clinical predictive value of virus genotype, menopausal status and mutational landscape in cervical cancer tissue using a NGS based human papillomavirus (HPV) assay and whole exome sequencing (WES)

Jean-Christophe Pignon, Heidi Giese, D. Foernzler, L. McDaniel, G. Bartha, J. Scheuenpflug, Zheng Feng
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引用次数: 0

Abstract

Purpose: Persistent HPV infections are associated with nearly all cervical cancers and some head & neck and genitourinary cancers. In cervical cancer, 14 high risk HPV genotypes have been previously identified with varying geographical prevalence and carcinogenicity. HPV16 and 18 account for >70% of cervical cancer incidence worldwide. There is an unmet need to explore HPV-associated cancer pathology, HPV infection status and molecular profiles to detect virus load and identify predictive gene signatures. We investigated the association between HPV genotypes and clinicopathological features and analyzed the mutational landscape using the ImmunoID NeXT Platform®. Methods: Early stage cervical cancer FFPE tissue samples (n=38) were analyzed. We detected and quantified oncoviral DNA, identified likely somatic mutations, and quantified genome-wide mutational burden. Any sample with at least one filtered read of HPV evidence was considered positive; zero such evidential reads were reported across a negative control cohort of > 439 non-cervical cancer samples. Oncovirus DNA counts and HPV genotype status were then evaluated against covariates (age; menopausal status) for statistical significance. Finally, mutation frequency was assessed in genes comprising major cervical cancer driver pathways from the KEGG and Biocarta databases. Results: Oncoviral HPV infections were detected using a NGS based approach in all tumor tissue with demonstrated robust assay performance. A statistically significant difference in viral DNA counts was observed between high risk genotypes HPV16 and 18 (n=27) and all other genotypes (n=10), (p=0.028, Student9s t). Genotypes were also significantly associated with menopausal status (p=0.01, Fisher9s Exact Test) and age at surgical resection (p=0.011, Student9s t). Among the pathways considered, TGF-β and MAP-kinase were the most frequently mutated across 38 samples and multiple pathway annotations. Conclusions: We applied a powerful NGS based WES approach that enables accurate detection of HPV genotypes with quantification of HPV viral DNA. This quantitative approach represents a possible promising clinical benefit over existing qualitative HPV genotyping assays and may have the potential for further development to define cancer type and treatment specific cutoff values for cancer prognosis. Furthermore, our results demonstrate that a WES based approach provides clinically valuable insights into the constitutive molecular mechanisms of cervical cancer. The association of HPV genotypes with clinical patient characteristics and/or mutational profiles has the potential to identify prognostic and predictive clinical biomarkers and to provide critical information for treatment defining strategies. Citation Format: Jean-Christophe Pignon, Heidi Giese, Dorothee Foernzler, Lee D. McDaniel, Gabor Bartha, Juergen Scheuenpflug, Zheng Feng. Investigating the potential clinical predictive value of virus genotype, menopausal status and mutational landscape in cervical cancer tissue using a NGS based human papillomavirus (HPV) assay and whole exome sequencing (WES) [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 363.
363:利用基于NGS的人乳头瘤病毒(HPV)检测和全外显子组测序(WES)研究宫颈癌组织中病毒基因型、绝经状态和突变格局的潜在临床预测价值
目的:持续HPV感染与几乎所有宫颈癌和一些头颈部和泌尿生殖系统癌有关。在宫颈癌中,14种高危HPV基因型已被确定,其地理患病率和致癌性各不相同。HPV16和hpv18占全世界宫颈癌发病率的70%。有一个未满足的需求,探索HPV相关的癌症病理,HPV感染状态和分子谱,以检测病毒载量和识别预测性基因特征。我们研究了HPV基因型与临床病理特征之间的关系,并使用ImmunoID NeXT Platform®分析了突变景观。方法:对38例早期宫颈癌FFPE组织标本进行分析。我们检测并量化了癌病毒DNA,确定了可能的体细胞突变,并量化了全基因组突变负担。任何至少有一个HPV过滤读数的样本都被认为是阳性的;在bbbb439例非宫颈癌样本的阴性对照队列中,没有报道这样的证据读数。然后评估癌病毒DNA计数和HPV基因型状态与协变量(年龄;绝经状态),没有统计学意义。最后,从KEGG和Biocarta数据库中评估了包括主要宫颈癌驱动通路的基因的突变频率。结果:使用基于NGS的方法在所有肿瘤组织中检测到HPV病毒感染,并显示出强大的检测性能。高危基因型HPV16和18 (n=27)与所有其他基因型(n=10)的病毒DNA计数差异有统计学意义(p=0.028, Student9s t)。基因型还与绝经状态(p=0.01, Fisher9s精确检验)和手术切除年龄(p=0.011, Student9s t)显著相关。在所考虑的38个样本和多个途径注释中,TGF-β和map -激酶是最常突变的。结论:我们应用了一种强大的基于NGS的WES方法,可以通过定量HPV病毒DNA来准确检测HPV基因型。与现有的定性HPV基因分型分析相比,这种定量方法可能具有很好的临床效益,并且可能具有进一步发展确定癌症类型和癌症预后治疗特异性临界值的潜力。此外,我们的研究结果表明,基于WES的方法为宫颈癌的组成分子机制提供了临床上有价值的见解。HPV基因型与临床患者特征和/或突变谱的关联有可能确定预后和预测性临床生物标志物,并为治疗确定策略提供关键信息。引文格式:Jean-Christophe Pignon, Heidi Giese, Dorothee Foernzler, Lee D. McDaniel, Gabor Bartha, Juergen Scheuenpflug,郑峰。利用基于NGS的人乳头瘤病毒(HPV)检测和全外显子组测序(WES)研究宫颈癌组织中病毒基因型、绝经状态和突变景观的潜在临床预测价值。见:美国癌症研究协会2021年年会论文集;2021年4月10日至15日和5月17日至21日。费城(PA): AACR;癌症杂志2021;81(13 -增刊):摘要第363期。
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