Utilization of primary tumor samples for cancer neoantigen discovery.

IF 10.3 1区医学 Q1 IMMUNOLOGY

Journal for Immunotherapy of Cancer Pub Date : 2025-01-11 DOI:10.1136/jitc-2024-010993

Vid Leko, Eric Groh, Shoshana T Levi, Amy R Copeland, Bradley Sinclair White, Billel Gasmi, Yong Li, Victoria Hill, Devikala Gurusamy, Noam Levin, Sanghyun Peter Kim, Sivasish Sindiri, Jared J Gartner, Todd D Prickett, Maria Parkhust, Frank J Lowery, Stephanie L Goff, Steven A Rosenberg, Paul Robbins

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引用次数: 0

Abstract

Background: The use of tumor-infiltrating T lymphocytes (TIL) that recognize cancer neoantigens has led to lasting remissions in metastatic melanoma and certain cases of metastatic epithelial cancer. For the treatment of the latter, selecting cells for therapy typically involves laborious screening of TIL for recognition of autologous tumor-specific mutations, detected through next-generation sequencing of freshly resected metastatic tumors. Our study explored the feasibility of using archived formalin-fixed, paraffin-embedded (FFPE) primary tumor samples for cancer neoantigen discovery, to potentially expedite this process and reduce the need for resections normally required for tumor sequencing.

Method: Whole-exome sequencing was conducted on matched primary and metastatic colorectal cancer samples from 22 patients. The distribution of metastatic tumor mutations that were confirmed as neoantigens through cognate TIL screening was evaluated in the corresponding primary tumors. Mutations unique to primary tumors were screened for recognition by metastasis-derived TIL and circulating T lymphocytes.

Results: We found that 25 (65.8%) of the 38 validated neoantigens identified in metastatic tumors from 18 patients with colorectal cancer were also present in matched primary tumor samples. This included all 12 neoantigens encoded by putative cancer driver genes, which are generally regarded as superior targets for adoptive cell therapy. The detection rate for other neoantigens, representing mutations without an established role in cancer biology, was 50% (13/26). Gene products encoding neoantigens detected in the primary tumors were not more likely to be clonal or broadly distributed among the analyzed metastatic lesions compared with those undetected in the primary tumors. Additionally, we found that mutations detected only in primary tumor samples did not elicit recognition by metastatic tumor-derived TIL but could elicit specific recognition by the autologous circulating memory T cells.

Conclusions: Our findings indicate that primary FFPE tumor-derived screening libraries could be used to discover most neoantigens present in metastatic tumors requiring treatment. Furthermore, this approach can reveal additional neoantigens not present in resected metastatic tumors, prompting further research to understand their clinical relevance as potential therapeutic targets.

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利用原始肿瘤样本发现癌症新抗原。

背景：使用肿瘤浸润T淋巴细胞（TIL）识别肿瘤新抗原已经导致转移性黑色素瘤和某些转移性上皮癌病例的持续缓解。对于后者的治疗，选择用于治疗的细胞通常需要费力地筛选TIL以识别自体肿瘤特异性突变，通过对新切除的转移性肿瘤进行下一代测序来检测。我们的研究探索了使用存档的福尔马林固定石蜡包埋（FFPE）原发肿瘤样本发现癌症新抗原的可行性，这可能会加快这一过程，并减少通常需要切除肿瘤测序的需要。方法：对22例匹配的原发性和转移性结直肠癌样本进行全外显子组测序。通过同源TIL筛查确认为新抗原的转移性肿瘤突变的分布在相应的原发肿瘤中进行评估。原发肿瘤特有的突变被转移源性TIL和循环T淋巴细胞筛选识别。结果：我们发现，在18例结直肠癌患者的转移性肿瘤中发现的38种有效新抗原中，有25种（65.8%）也存在于匹配的原发肿瘤样本中。这包括所有12种由假定的癌症驱动基因编码的新抗原，它们通常被认为是过继细胞治疗的优越靶点。其他新抗原（代表在癌症生物学中没有确定作用的突变）的检出率为50%（13/26）。与原发肿瘤中未检测到的基因产物相比，在原发肿瘤中检测到的编码新抗原的基因产物在分析的转移灶中不太可能是克隆的或广泛分布的。此外，我们发现仅在原发肿瘤样本中检测到的突变不会引起转移性肿瘤来源的TIL的识别，但可以引起自体循环记忆T细胞的特异性识别。结论：我们的研究结果表明，原发性FFPE肿瘤来源的筛选文库可用于发现需要治疗的转移性肿瘤中存在的大多数新抗原。此外，这种方法可以揭示在切除的转移性肿瘤中不存在的其他新抗原，促使进一步研究了解它们作为潜在治疗靶点的临床相关性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal for Immunotherapy of Cancer Biochemistry, Genetics and Molecular Biology-Molecular Medicine

CiteScore

17.70

自引率

4.60%

发文量

522

审稿时长

18 weeks

期刊介绍： The Journal for ImmunoTherapy of Cancer (JITC) is a peer-reviewed publication that promotes scientific exchange and deepens knowledge in the constantly evolving fields of tumor immunology and cancer immunotherapy. With an open access format, JITC encourages widespread access to its findings. The journal covers a wide range of topics, spanning from basic science to translational and clinical research. Key areas of interest include tumor-host interactions, the intricate tumor microenvironment, animal models, the identification of predictive and prognostic immune biomarkers, groundbreaking pharmaceutical and cellular therapies, innovative vaccines, combination immune-based treatments, and the study of immune-related toxicity.