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免疫治疗中纳武利尤单抗的肿瘤生态系统的新抗原免疫原性景观和演变。

Neoantigen immunogenicity landscapes and evolution of tumor ecosystems during immunotherapy with nivolumab.

机构信息

Center for Immunotherapy and Precision Immuno-Oncology, Cleveland Clinic, Cleveland, OH, USA.

Lerner Research Institute, Cleveland Clinic, Cleveland, OH, USA.

出版信息

Nat Med. 2024 Nov;30(11):3209-3222. doi: 10.1038/s41591-024-03240-y. Epub 2024 Sep 30.

Abstract

Neoantigen immunoediting drives immune checkpoint blockade efficacy, yet the molecular features of neoantigens and how neoantigen immunogenicity shapes treatment response remain poorly understood. To address these questions, 80 patients with non-small cell lung cancer were enrolled in the biomarker cohort of CheckMate 153 (CA209-153), which collected radiographic guided biopsy samples before treatment and during treatment with nivolumab. Early loss of mutations and neoantigens during therapy are both associated with clinical benefit. We examined 1,453 candidate neoantigens, including many of which that had reduced cancer cell fraction after treatment with nivolumab, and identified 196 neopeptides that were recognized by T cells. Mapping these neoantigens to clonal dynamics, evolutionary trajectories and clinical response revealed a strong selection against immunogenic neoantigen-harboring clones. We identified position-specific amino acid and physiochemical features related to immunogenicity and developed an immunogenicity score. Nivolumab-induced microenvironmental evolution in non-small cell lung cancer shared some similarities with melanoma, yet critical differences were apparent. This study provides unprecedented molecular portraits of neoantigen landscapes underlying nivolumab's mechanism of action.

摘要

新抗原免疫编辑驱动免疫检查点阻断疗效,但新抗原的分子特征以及新抗原免疫原性如何影响治疗反应仍知之甚少。为了解决这些问题,80 名非小细胞肺癌患者被纳入 CheckMate 153(CA209-153)的生物标志物队列,该队列在治疗前和接受nivolumab 治疗期间收集影像学引导的活检样本。治疗过程中早期突变和新抗原的丢失均与临床获益相关。我们检查了 1453 个候选新抗原,包括许多在接受 nivolumab 治疗后癌细胞分数降低的新抗原,并鉴定了 196 个被 T 细胞识别的新肽。将这些新抗原映射到克隆动力学、进化轨迹和临床反应上,揭示了对免疫原性新抗原携带克隆的强烈选择。我们确定了与免疫原性相关的位置特异性氨基酸和物理化学特征,并开发了一个免疫原性评分。非小细胞肺癌中 nivolumab 诱导的微环境进化与黑色素瘤有一些相似之处,但也存在明显的差异。本研究提供了 nivolumab 作用机制下新抗原景观的前所未有的分子特征。

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