Indication-specific tumor evolution and its impact on neoantigen targeting and biomarkers for individualized cancer immunotherapies

Amy A Lo; Andrew Wallace; Daniel OreperNicolas LounsburyCharles HavnarXimo Pechuan-JorgeThomas D WuRichard BourgonRyan JonesKatrina KroghGuang-Yu YangOliver A Zill

首页> 外文期刊>journal for immunotherapy of cancer >Indication-specific tumor evolution and its impact on neoantigen targeting and biomarkers for individualized cancer immunotherapies

【24h】

Indication-specific tumor evolution and its impact on neoantigen targeting and biomarkers for individualized cancer immunotherapies

机译：Indication-specific tumor evolution and its impact on neoantigen targeting and biomarkers for individualized cancer immunotherapies

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相关主题

摘要

Background Individualized neoantigen-specific immunotherapy (iNeST) requires robustly expressed clonal neoantigens for efficacy, but tumor mutational heterogeneity, loss of neoantigen expression, and variable tissue sampling present challenges. It is assumed that clonal neoantigens are preferred targets for immunotherapy, but the distributions of clonal neoantigens are not well characterized across cancer types. Methods We combined multiregion sequencing (MR-seq) analysis of five untreated, synchronously sampled metastatic solid tumors with re-analysis of published MR-seq data from 103 patients in order to characterize their globally clonal neoantigen content and factors that would impact neoantigen targeting. Results Branching evolution in colorectal cancer and renal cell carcinoma led to fewer clonal neoantigens and to clade-specific neoantigens (those shared across a subset of tumor regions but not fully clonal), with the latter not being readily distinguishable in single tumor samples. In colorectal, renal, and bladder cancer, most tumors had few globally clonal neoantigens. Prioritizing mutations with higher purity-adjusted and ploidy-adjusted variant allele frequency enriched for globally clonal neoantigens (those found in all tumor regions), whereas estimated cancer cell fraction derived from clustering-based tools, surprisingly, did not. Neoantigen quality was associated with loss of neoantigen expression in the bladder cancer case, and HLA-allele loss was observed in the renal and non-small cell lung cancer cases. Conclusions We show that tumor type, multilesion sampling, neoantigen expression, and HLA allele retention are important factors for iNeST targeting and patient selection, and may also be important factors to consider in the development of biomarker strategies.

著录项

来源
《journal for immunotherapy of cancer》 |2021年第10期|1-13|共13页
作者
Amy A Lo; Andrew Wallace; Daniel OreperNicolas LounsburyCharles HavnarXimo Pechuan-JorgeThomas D WuRichard BourgonRyan JonesKatrina KroghGuang-Yu YangOliver A Zill;
展开▼
作者单位

Department of Research Pathology, Genentech Inc;

Department of Oncology Bioinformatics, Genentech Inc;

Department of Cancer Immunology, Genentech IncDepartment of Pathology, Northwestern UniversityCurrent affiliation, init.bio, Inc;

展开▼
收录信息
原文格式 PDF
正文语种英语
中图分类
关键词
antigen-mediated; antigens; biomarkers; clonal selection; computational biology; neoplasm; tumor; urinary bladder neoplasms;

Indication-specific tumor evolution and its impact on neoantigen targeting and biomarkers for individualized cancer immunotherapies

摘要

著录项

相关主题

期刊订阅