Driver mutations in GNAQ and GNA11 genes as potential targets for precision immunotherapy in uveal melanoma patients

IF 6.5 2区 医学 Q1 IMMUNOLOGY
Sandra García-Mulero, Roberto Fornelino, Marco Punta, Stefano Lise, Mar Varela, Luis P. del Carpio, Rafael Moreno, Marcel Costa-García, Dietmar Rieder, Zlatko Trajanoski, Alena Gros, Ramón Alemany, Josep María Piulats, Rebeca Sanz-Pamplona
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Abstract

Uveal melanoma (UM) is the most common ocular malignancy in adults. Nearly 95% of UM patients carry the mutually exclusive mutations in the homologous genes GNAQ (amino acid change Q209L/Q209P) and GNA11 (aminoacid change Q209L). UM is located in an immunosuppressed organ and does not suffer immunoediting. Therefore, we hypothesize that driver mutations in GNAQ/11 genes could be recognized by the immune system. Genomic and transcriptomic data from primary uveal tumors were collected from the TCGA-UM dataset (n = 80) and used to assess the immunogenic potential for GNAQ/GNA11 Q209L/Q209P mutations using a variety of tools and HLA type information. All prediction tools showed stronger GNAQ/11 Q209L binding to HLA than GNAQ/11 Q209P. The immunogenicity analysis revealed that Q209L is likely to be presented by more than 73% of individuals in 1000 G databases whereas Q209P is only predicted to be presented in 24% of individuals. GNAQ/11 Q209L showed a higher likelihood to be presented by HLA-I molecules than almost all driver mutations analyzed. Finally, samples carrying Q209L had a higher immune-reactive phenotype. Regarding cancer risk, seven HLA genotypes with low Q209L affinity show higher frequency in uveal melanoma patients than in the general population. However, no clear association was found between any HLA genotype and survival. Results suggest a high potential immunogenicity of the GNAQ/11 Q209L variant that could allow the generation of novel therapeutic tools to treat UM like neoantigen vaccinations.
GNAQ和GNA11基因驱动突变作为葡萄膜黑色素瘤患者精确免疫治疗的潜在靶点
葡萄膜黑色素瘤(Uveal melanoma, UM)是成人最常见的眼部恶性肿瘤。近95%的UM患者携带同源基因GNAQ(氨基酸变化Q209L/Q209P)和GNA11(氨基酸变化Q209L)互异突变。UM位于免疫抑制器官中,不受免疫编辑。因此,我们假设GNAQ/11基因的驱动突变可以被免疫系统识别。从TCGA-UM数据集中收集原发性葡萄膜肿瘤的基因组和转录组学数据(n = 80),并使用各种工具和HLA类型信息评估GNAQ/GNA11 Q209L/Q209P突变的免疫原性潜力。所有预测工具均显示GNAQ/11 Q209L与HLA的结合强于GNAQ/11 Q209P。免疫原性分析显示,在1000个G数据库中,Q209L可能在73%以上的个体中出现,而Q209P预计仅在24%的个体中出现。GNAQ/ 11q209l显示hla - 1分子呈现的可能性高于几乎所有分析的驱动突变。最后,携带Q209L的样本具有更高的免疫反应表型。在癌症风险方面,7种Q209L亲和力较低的HLA基因型在葡萄膜黑色素瘤患者中的出现频率高于普通人群。然而,没有发现任何HLA基因型与生存率之间的明确关联。结果表明,GNAQ/11 Q209L变体具有很高的潜在免疫原性,可以产生新的治疗工具来治疗UM,如新抗原疫苗接种。
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来源期刊
Oncoimmunology
Oncoimmunology ONCOLOGYIMMUNOLOGY-IMMUNOLOGY
CiteScore
12.50
自引率
2.80%
发文量
276
审稿时长
24 weeks
期刊介绍: OncoImmunology is a dynamic, high-profile, open access journal that comprehensively covers tumor immunology and immunotherapy. As cancer immunotherapy advances, OncoImmunology is committed to publishing top-tier research encompassing all facets of basic and applied tumor immunology. The journal covers a wide range of topics, including: -Basic and translational studies in immunology of both solid and hematological malignancies -Inflammation, innate and acquired immune responses against cancer -Mechanisms of cancer immunoediting and immune evasion -Modern immunotherapies, including immunomodulators, immune checkpoint inhibitors, T-cell, NK-cell, and macrophage engagers, and CAR T cells -Immunological effects of conventional anticancer therapies.
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