| Literature DB >> 32086382 |
Tianshi Lu1, Shidan Wang1, Lin Xu1,2, Qinbo Zhou1, Nirmish Singla3,4, Jianjun Gao5, Subrata Manna6, Laurentiu Pop6, Zhiqun Xie1, Mingyi Chen7, Jason J Luke8, James Brugarolas4,9, Raquibul Hannan4,6, Tao Wang10,4.
Abstract
Lack of responsiveness to checkpoint inhibitors is a central problem in the modern era of cancer immunotherapy. Tumor neoantigens are critical targets of the host antitumor immune response, and their presence correlates with the efficacy of immunotherapy treatment. Many studies involving assessment of tumor neoantigens principally focus on total neoantigen load, which simplistically treats all neoantigens equally. Neoantigen load has been linked with treatment response and prognosis in some studies but not others. We developed a Cauchy-Schwarz index of Neoantigens (CSiN) score to better account for the degree of concentration of immunogenic neoantigens in truncal mutations. Unlike total neoantigen load determinations, CSiN incorporates the effect of both clonality and MHC binding affinity of neoantigens when characterizing tumor neoantigen profiles. By analyzing the clinical responses in 501 treated patients with cancer (with most receiving checkpoint inhibitors) and the overall survival of 1978 patients with cancer at baseline, we showed that CSiN scores predict treatment response to checkpoint inhibitors and prognosis in patients with melanoma, lung cancer, and kidney cancer. CSiN score substantially outperformed prior genetics-based prediction methods of responsiveness and fills an important gap in research involving assessment of tumor neoantigen burden.Entities:
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Year: 2020 PMID: 32086382 PMCID: PMC7239327 DOI: 10.1126/sciimmunol.aaz3199
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468