Dynamic modulation of claudin18.2 expression and remodeling of the tumor microenvironment in gastric cancer during chemo-immunotherapy.

IF 10.6 1区医学 Q1 IMMUNOLOGY

Journal for Immunotherapy of Cancer Pub Date : 2025-09-29 DOI:10.1136/jitc-2025-012683

Sung Hee Lim, Takeshi Kuwata, Minae An, Jung Yong Hong, Seung Tae Kim, Yuki Matsubara, Kohei Shitara, Jeeyun Lee

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Abstract

Background: Claudin 18.2 (CLDN18.2) is a tight junction protein retained in malignant transformation of gastric cancer (GC) and is a promising therapeutic target. Despite the clinical benefit of zolbetuximab in CLDN18.2-positive tumors, the dynamic expression of CLDN18.2 during chemoimmunotherapy and its implications in the tumor microenvironment (TME) remain poorly understood.

Methods: In a prospective single-arm phase II trial, we evaluated serial tumor biopsies from patients with advanced GC receiving first-line chemotherapy (capecitabine/oxaliplatin) with sequential pembrolizumab. CLDN18.2 expression was assessed by immunohistochemistry, and integrated molecular analyses-including whole transcriptome, whole exome, and single-cell RNA sequencing-were performed to explore TME alterations and molecular correlates.

Results: Among 57 patients, 40.4% were CLDN18.2-positive at baseline. CLDN18.2 positivity was associated with diffuse-type histology, higher programmed death-ligand 1 (PD-L1) combined positive scores, and an immune-inflamed, stroma-rich TME characterized by enhanced T cell infiltration, transforming growth factor-β signaling, and matrix remodeling. Gene set enrichment analyses revealed immune activation and stromal remodeling in CLDN18.2-positive tumors. Single-cell analysis showed increased regulatory T cells and galectin-3-CD44 signaling in CLDN18.2-positive tumors. After one cycle of chemotherapy, CLDN18.2 expression was lost in 40% of initially positive tumors, while 10% of initially negative tumors gained expression-particularly in fibrotic TMEs. Survival outcomes were not significantly different between CLDN18.2-positive and CLDN18.2-negative groups; however, patients negative for both CLDN18.2 and PD-L1 showed poorer prognosis.

Conclusions: CLDN18.2 expression is dynamically regulated during chemoimmunotherapy and is associated with a distinct immunosuppressive and fibrotic TME. These findings highlight the importance of repeated biomarker assessment and suggest potential combinatorial therapeutic strategies targeting both epithelial and stromal compartments in GC.

Trial registration number: NCT04249739.

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化疗-免疫治疗期间胃癌组织中claudin18.2表达的动态调控及肿瘤微环境的重塑。

背景：Claudin 18.2 （CLDN18.2）是胃癌（GC）恶性转化中保留的紧密连接蛋白，是一种有前景的治疗靶点。尽管zolbetuximab在CLDN18.2阳性肿瘤中的临床获益，但在化疗免疫治疗期间CLDN18.2的动态表达及其在肿瘤微环境（TME）中的意义仍然知之甚少。方法：在一项前瞻性单臂II期试验中，我们评估了接受一线化疗（卡培他滨/奥沙利铂）和序贯派姆单抗的晚期胃癌患者的连续肿瘤活检。通过免疫组织化学评估CLDN18.2的表达，并进行综合分子分析，包括全转录组、全外显子组和单细胞RNA测序，以探索TME改变和分子相关性。结果：57例患者中，40.4%基线时cldn18.2阳性。CLDN18.2阳性与弥漫性组织学、较高的程序性死亡配体1 （PD-L1）联合阳性评分以及以T细胞浸润增强、转化生长因子-β信号传导和基质重塑为特征的免疫炎症、基质丰富的TME相关。基因集富集分析揭示了cldn18.2阳性肿瘤的免疫激活和基质重塑。单细胞分析显示，在cldn18.2阳性肿瘤中，调节性T细胞和半凝集素-3- cd44信号传导增加。一个化疗周期后，40%的初始阳性肿瘤中CLDN18.2表达丧失，而10%的初始阴性肿瘤获得表达，尤其是在纤维化TMEs中。cldn18.2阳性组和cldn18.2阴性组的生存结局无显著差异；然而，CLDN18.2和PD-L1均阴性的患者预后较差。结论：CLDN18.2的表达在化疗免疫治疗过程中受到动态调节，并与明显的免疫抑制和纤维化性TME相关。这些发现强调了重复生物标志物评估的重要性，并提出了针对胃癌上皮和间质室的潜在联合治疗策略。试验注册号：NCT04249739。

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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.