Tumour-wide RNA splicing aberrations generate actionable public neoantigens

IF 50.5 1区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES Nature Pub Date : 2025-02-19 DOI:10.1038/s41586-024-08552-0

Darwin W. Kwok, Nicholas O. Stevers, Iñaki Etxeberria, Takahide Nejo, Maggie Colton Cove, Lee H. Chen, Jangham Jung, Kaori Okada, Senthilnath Lakshmanachetty, Marco Gallus, Abhilash Barpanda, Chibo Hong, Gary K. L. Chan, Jerry Liu, Samuel H. Wu, Emilio Ramos, Akane Yamamichi, Payal B. Watchmaker, Hirokazu Ogino, Atsuro Saijo, Aidan Du, Nadia R. Grishanina, James Woo, Aaron Diaz, Shawn L. Hervey-Jumper, Susan M. Chang, Joanna J. Phillips, Arun P. Wiita, Christopher A. Klebanoff, Joseph F. Costello, Hideho Okada

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Abstract

T cell-based immunotherapies hold promise in treating cancer by leveraging the immune system’s recognition of cancer-specific antigens¹. However, their efficacy is limited in tumours with few somatic mutations and substantial intratumoural heterogeneity^2,3,4. Here we introduce a previously uncharacterized class of tumour-wide public neoantigens originating from RNA splicing aberrations in diverse cancer types. We identified T cell receptor clones capable of recognizing and targeting neoantigens derived from aberrant splicing in GNAS and RPL22. In cases with multi-site biopsies, we detected the tumour-wide expression of the GNAS neojunction in glioma, mesothelioma, prostate cancer and liver cancer. These neoantigens are endogenously generated and presented by tumour cells under physiologic conditions and are sufficient to trigger cancer cell eradication by neoantigen-specific CD8⁺ T cells. Moreover, our study highlights a role for dysregulated splicing factor expression in specific cancer types, leading to recurrent patterns of neojunction upregulation. These findings establish a molecular basis for T cell-based immunotherapies addressing the challenges of intratumoural heterogeneity.

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基于 T 细胞的免疫疗法可利用免疫系统对癌症特异性抗原的识别能力来治疗癌症1。然而，这些疗法在体细胞突变较少且瘤内异质性较大的肿瘤中疗效有限2,3,4。在这里，我们介绍了一类以前未曾描述过的全肿瘤公共新抗原，其来源于不同癌症类型中的 RNA 剪接畸变。我们发现的 T 细胞受体克隆能够识别并靶向源自 GNAS 和 RPL22 中异常剪接的新抗原。在多部位活检的病例中，我们在胶质瘤、间皮瘤、前列腺癌和肝癌中检测到全肿瘤范围的 GNAS 新连接表达。这些新抗原是肿瘤细胞在生理条件下内源性产生和表达的，足以引发新抗原特异性 CD8+ T 细胞消灭癌细胞。此外，我们的研究还强调了剪接因子表达失调在特定癌症类型中的作用，这导致了新连接上调的反复模式。这些发现为基于 T 细胞的免疫疗法应对瘤内异质性挑战奠定了分子基础。

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来源期刊

Nature 综合性期刊-综合性期刊

CiteScore

90.00

自引率

1.20%

发文量

3652

审稿时长

3 months

期刊介绍： Nature is a prestigious international journal that publishes peer-reviewed research in various scientific and technological fields. The selection of articles is based on criteria such as originality, importance, interdisciplinary relevance, timeliness, accessibility, elegance, and surprising conclusions. In addition to showcasing significant scientific advances, Nature delivers rapid, authoritative, insightful news, and interpretation of current and upcoming trends impacting science, scientists, and the broader public. The journal serves a dual purpose: firstly, to promptly share noteworthy scientific advances and foster discussions among scientists, and secondly, to ensure the swift dissemination of scientific results globally, emphasizing their significance for knowledge, culture, and daily life.

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