PD-1-Positive CD8+ T Cells and PD-1-Positive FoxP3+ Cells in Tumor Microenvironment Predict Response to Neoadjuvant Chemoimmunotherapy in Gastric Cancer Patients.

IF 4.4 2区医学 Q1 ONCOLOGY

Cancers Pub Date : 2025-07-21 DOI:10.3390/cancers17142407

Liubov A Tashireva, Anna Yu Kalinchuk, Elena O Shmakova, Elisaveta A Tsarenkova, Dmitriy M Loos, Pavel Iamschikov, Ivan A Patskan, Alexandra V Avgustinovich, Sergey V Vtorushin, Irina V Larionova, Evgeniya S Grigorieva

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Abstract

Background/objectives: In gastric cancer, only a subset of patients benefit clinically from neoadjuvant chemoimmunotherapy, underscoring the need for robust biomarkers that can predict treatment responses and guide personalized immunotherapy. This study aimed to characterize the immune microenvironment of gastric tumors and identify predictive markers associated with therapeutic efficacy.

Methods: We prospectively enrolled 16 patients with histologically confirmed, PD-L1-positive (CPS ≥ 1) gastric adenocarcinoma (T_2-4N_0-1M₀). All patients received eight cycles of FLOT chemotherapy combined with pembrolizumab. Treatment response was assessed by Mandard tumor regression grading. Spatial transcriptomic profiling (10x Genomics Visium) and multiplex immunofluorescence were used to evaluate tumor-infiltrating immune cell subsets and PD-1 expression at baseline and after treatment.

Results: Transcriptomic analysis differentiated the immune landscapes of responders from non-responders. Responders exhibited elevated expression of IL1B, CXCL5, HMGB1, and IFNGR2, indicative of an inflamed tumor microenvironment and type I/II interferon signaling. In contrast, non-responders demonstrated upregulation of immunosuppressive genes such as LGALS3, IDO1, and CD55, along with enrichment in oxidative phosphorylation and antigen presentation pathways. Multiplex immunofluorescence confirmed a higher density of FoxP3⁺ regulatory T cells in non-responders (median 5.36% vs. 2.41%; p = 0.0032). Notably, PD-1⁺ CD8⁺ T cell and PD-1⁺ FoxP3⁺ Treg frequencies were significantly elevated in non-responders, suggesting that PD-1 expression within cytotoxic and regulatory compartments may contribute to immune evasion. No substantial differences were observed in PD-L1 CPS or PD-1⁺ B cells and PD-1⁺ macrophages.

Conclusions: Our findings identify PD-1⁺ CD8⁺ T cells and PD-1⁺ FoxP3⁺ Tregs as potential biomarkers of resistance to neoadjuvant chemoimmunotherapy in gastric cancer. Transcriptional programs centered on IL1B/CXCL5 and LGALS3/IDO1 define distinct immune phenotypes that may guide future combination strategies targeting both effector and suppressive arms of the tumor immune response.

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肿瘤微环境中pd -1阳性CD8+ T细胞和pd -1阳性FoxP3+细胞预测胃癌患者对新辅助化疗免疫治疗的反应

背景/目的：在胃癌中，只有一小部分患者从新辅助化疗免疫治疗中获益，这强调了对能够预测治疗反应和指导个性化免疫治疗的强大生物标志物的需求。本研究旨在表征胃肿瘤的免疫微环境，并确定与治疗效果相关的预测标志物。方法：前瞻性纳入16例组织学证实的pd - l1阳性（CPS≥1）胃腺癌（T2-4N0-1M0）患者。所有患者均接受了8个周期的FLOT化疗联合派姆单抗。采用标准肿瘤消退分级评估治疗效果。使用空间转录组分析（10x Genomics Visium）和多重免疫荧光来评估基线和治疗后肿瘤浸润免疫细胞亚群和PD-1表达。结果：转录组学分析区分了应答者和无应答者的免疫景观。应答者表现出IL1B、CXCL5、HMGB1和IFNGR2的表达升高，表明肿瘤微环境炎症和I/II型干扰素信号传导。相反，无应答者表现出免疫抑制基因如LGALS3、IDO1和CD55的上调，以及氧化磷酸化和抗原递呈途径的富集。多重免疫荧光证实无应答者中FoxP3+调节性T细胞密度更高(中位数5.36% vs. 2.41%；P = 0.0032)。值得注意的是，PD-1+ CD8+ T细胞和PD-1+ FoxP3+ Treg频率在无应答者中显著升高，这表明细胞毒性和调节区内PD-1的表达可能有助于免疫逃避。PD-L1 CPS、PD-1+ B细胞和PD-1+巨噬细胞均无显著差异。结论：我们的研究结果确定了PD-1+ CD8+ T细胞和PD-1+ FoxP3+ Tregs是胃癌新辅助化疗免疫治疗耐药的潜在生物标志物。以IL1B/CXCL5和LGALS3/IDO1为中心的转录程序定义了不同的免疫表型，这可能指导未来针对肿瘤免疫反应的效应臂和抑制臂的联合策略。

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来源期刊

Cancers Medicine-Oncology

CiteScore

8.00

自引率

9.60%

发文量

5371

审稿时长

18.07 days

期刊介绍： Cancers (ISSN 2072-6694) is an international, peer-reviewed open access journal on oncology. It publishes reviews, regular research papers and short communications. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced.