Progressive natural killer cell dysfunction in advanced-stage clear-cell renal cell carcinoma and association with clinical outcomes.

IF 7.1 2区医学 Q1 ONCOLOGY ESMO Open Pub Date : 2025-01-14 DOI:10.1016/j.esmoop.2024.104105

W Xu, G Birch, A Meliki, V Moritz, M Bharadwaj, N R Schindler, C Labaki, R M Saliby, K Dinh, J T Horst, M Sun, S Kashima, M Hugaboom, A Dighe, M Machaalani, G-S M Lee, M Hurwitz, B A McGregor, M S Hirsch, S A Shukla, D F McDermott, S Signoretti, R Romee, T K Choueiri, D A Braun

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Abstract

Background: Natural killer (NK) cells are important contributors to antitumor immunity in clear-cell renal cell carcinoma (ccRCC). However, their phenotype, function, and association with clinical outcomes in ccRCC remain poorly understood.

Materials and methods: We analyzed single-cell RNA sequencing data from 13 primary tumors, 1 localized tumor extension, and 1 metastasis from ccRCC patients at different clinical stages. For each primary tumor specimen, paired normal kidneys were also analyzed. Differential gene expression analysis was carried out to investigate NK cell phenotypes and to derive a gene expression signature. Gene signatures from NK cell subclusters of interest were used to interrogate bulk transcriptomic datasets and expression with clinical outcomes. Finally, tumor-infiltrating NK cell function (cytokine production and cytotoxicity) was assessed by isolation of live NK cells from ccRCC tissue, co-culture with K562 target cells, and measurement of cytokine production (interferon-γ) and cytotoxicity (CD107a) markers by flow cytometry.

Results: Single-cell transcriptomic data were analyzed from 13 patients with ccRCC (tumor/normal kidney), resulting in 21 139 NK cells. Clustering analysis revealed six NK cell subsets. Bright-like NK cells were significantly enriched in advanced ccRCC compared with localized ccRCC and normal kidney, expressed markers of tissue residency (ZNF683/Hobit, ITGA1/CD49a, CD9, ITGAE/CD103), and had decreased expression of cytotoxicity genes (GZMB/Granzyme-B, PRF1/perforin). In independent cohorts (The Cancer Genome Atlas ccRCC cohort, CheckMate 025), a gene expression score representing this dysfunctional NK cell phenotype was enriched in advanced ccRCC and was associated with worse overall survival. Functional interrogation of tumor-infiltrating NK cells from ccRCC confirmed that tumor-resident CD49a+CD9+ NK cells had impaired cytotoxicity compared with CD49a-CD9- NK cells.

Conclusions: A dysfunctional, tumor-resident NK cell phenotype was enriched among patients with metastatic disease and associated with worse survival in patients with advanced ccRCC across multiple patient cohorts. Restoration of NK cell function (via cytokine stimulation or NK cell engineering) could provide a novel avenue for therapeutic intervention against ccRCC.

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晚期透明细胞肾细胞癌的进行性自然杀伤细胞功能障碍及其与临床结果的关系

背景：自然杀伤细胞（NK）是透明细胞肾细胞癌（ccRCC）抗肿瘤免疫的重要贡献者。然而，它们在ccRCC中的表型、功能和与临床结果的关联仍然知之甚少。材料和方法：我们分析了13例原发性肿瘤、1例局部肿瘤扩展和1例不同临床阶段的ccRCC患者的单细胞RNA测序数据。对于每个原发肿瘤标本，配对正常肾脏也进行了分析。差异基因表达分析进行研究NK细胞表型，并得出基因表达特征。来自感兴趣的NK细胞亚群的基因签名被用来询问大量转录组数据集和临床结果的表达。最后，通过从ccRCC组织中分离活NK细胞，与K562靶细胞共培养，并通过流式细胞术测量细胞因子产生（干扰素-γ）和细胞毒性（CD107a）标志物，评估肿瘤浸润NK细胞的功能（细胞因子产生和细胞毒性）。结果：对13例ccRCC（肿瘤/正常肾）患者的单细胞转录组学数据进行了分析，结果显示有21 139个NK细胞。聚类分析显示有6个NK细胞亚群。与局部ccRCC和正常肾脏相比，晚期ccRCC中亮样NK细胞显著富集，表达组织居住标志物（ZNF683/Hobit、ITGA1/CD49a、CD9、ITGAE/CD103），细胞毒性基因（GZMB/Granzyme-B、PRF1/perforin）表达降低。在独立队列中（Cancer Genome Atlas ccRCC队列，CheckMate 025），代表这种功能失调NK细胞表型的基因表达评分在晚期ccRCC中富集，并且与较差的总生存率相关。对来自ccRCC的肿瘤浸润NK细胞的功能调查证实，与CD49a-CD9- NK细胞相比，肿瘤驻留CD49a+CD9+ NK细胞的细胞毒性受损。结论：在多个患者队列中，转移性疾病患者中功能失调的肿瘤驻留NK细胞表型丰富，并且与晚期ccRCC患者的较差生存率相关。恢复NK细胞功能（通过细胞因子刺激或NK细胞工程）可能为治疗ccRCC提供新的途径。

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来源期刊

ESMO Open Medicine-Oncology

CiteScore

11.70

自引率

2.70%

发文量

255

审稿时长

10 weeks

期刊介绍： ESMO Open is the online-only, open access journal of the European Society for Medical Oncology (ESMO). It is a peer-reviewed publication dedicated to sharing high-quality medical research and educational materials from various fields of oncology. The journal specifically focuses on showcasing innovative clinical and translational cancer research. ESMO Open aims to publish a wide range of research articles covering all aspects of oncology, including experimental studies, translational research, diagnostic advancements, and therapeutic approaches. The content of the journal includes original research articles, insightful reviews, thought-provoking editorials, and correspondence. Moreover, the journal warmly welcomes the submission of phase I trials and meta-analyses. It also showcases reviews from significant ESMO conferences and meetings, as well as publishes important position statements on behalf of ESMO. Overall, ESMO Open offers a platform for scientists, clinicians, and researchers in the field of oncology to share their valuable insights and contribute to advancing the understanding and treatment of cancer. The journal serves as a source of up-to-date information and fosters collaboration within the oncology community.