脂质摄取在卵巢癌微环境诱导CD4+调节性T细胞表达PD-1/CTLA-4中的作用研究

脂质摄取在卵巢癌微环境诱导CD4+调节性T细胞表达PD-1/CTLA-4中的作用研究
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作者单位:江苏省人民医院(南京医科大学第一附属医院)
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基金项目:国家自然科学基金；江苏省自然科学基金项目；南京医科大学齐鲁临床研究基金；江苏省人民医院妇幼高质量发展基础研究面上项目

The Role of Lipid Uptake in the Ovarian Cancer Microenvironment-Induced Expression of PD-1/CTLA-4 in CD4+ Regulatory T Cells

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1.Jiangsu Provincial People'2.'3.s Hospital (The First Affiliated Hospital of Nanjing Medical University)

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National Natural Science Foundation of China (NSFC); Natural Science Foundation of Jiangsu Province; Qilu Clinical Research Fund of Nanjing Medical University; General Program for High-Quality Development of Maternal and Child Health at Jiangsu Provincial People's Hospital

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摘要：目的：本研究旨在探究卵巢癌（Ovarian cancer, OV）浸润性调节性CD4+T细胞（regulatory T cells, CD4+Tregs）的脂质摄取与积累情况，及其与CD4+Tregs中PD-1/CTLA-4表达的相关性。方法：采用亲脂性荧光染料BODIPY? 493/503和荧光脂肪酸探针BODIPY? 500/510 C1 C12分别检测从卵巢癌组织或与不同卵巢癌细胞系（ES-2, SKOV3, CAOV3）上清共培养的人源CD4+Tregs的细胞内脂质含量和脂质摄取能力；使用脂肪酸氧化抑制剂（Etomoxir）、脂肪酸合成抑制剂（C75）和脂肪酸摄取抑制剂（磺基-N-琥珀酰亚胺油酸酯，SSO）干预脂质代谢；通过流式细胞术分析CD4+Tregs上免疫抑制分子PD-1和CTLA-4的表达。结果：卵巢癌组织浸润性CD4+Tregs相较于传统CD4+T细胞（Conventional T cells, Tconv）表现出更高的脂质含量和脂质摄取能力（P < 0.01）。在体外实验中，与基础培养基相比，卵巢癌细胞培养上清（Tumor Supernatants，TSNs）可显著提升CD4+Tregs的胞内脂质含量与摄取能力（P < 0.05），其中CAOV3来源上清的作用最为显著。此外，CAOV3上清还能提升CD4+Tregs上PD-1与CTLA-4的表达（P < 0.05）。CD4+Tregs的脂质积累随CAOV3上清浓度增加呈剂量依赖性上升（P < 0.05），且其对胞外荧光脂肪酸类似物的摄取能力具有浓度依赖性增强（P < 0.05）。脂肪酸摄取抑制剂SSO可有效逆转CAOV3上清诱导的CD4+Tregs脂质积累（P < 0.05）及PD-1（P < 0.01）、CTLA-4（P < 0.05）的高表达；而脂肪酸氧化抑制剂Etomoxir与合成抑制剂C75则无显著影响。结论：卵巢癌微环境通过促进CD4+Tregs的脂质摄取，提高其细胞内脂质含量，促进其免疫抑制分子PD-1和CTLA-4表达。靶向脂肪酸摄取途径可能是逆转卵巢癌中Tregs介导的免疫抑制的潜在策略。关键词：卵巢癌；CD4+Tregs；脂质；PD-1/CTLA-4

Abstract:

Abstract: Objective: This study aimed to investigate the lipid metabolism characteristics, particularly lipid uptake and accumulation, of regulatory CD4+ T cells (Tregs) in the ovarian cancer microenvironment, and its potential impact on their PD-1/CTLA-4. Methods: The lipophilic fluorescent dye BODIPY? 493/503 and the fluorescent fatty acid probe BODIPY? 500/510 C1 C12 were used to detect intracellular lipid content and lipid uptake capacity, respectively, in human CD4+Tregs isolated from ovarian cancer tissues or co-cultured with supernatants from various ovarian cancer cell lines (ES-2, SKOV3, CAOV3). Lipid metabolism was modulated using the fatty acid oxidation inhibitor Etomoxir, the fatty acid synthesis inhibitor C75, and the fatty acid uptake inhibitor Sulfo-N-succinimidyl oleate (SSO). Lipid content and the expression of immunosuppressive molecules PD-1 and CTLA-4 were analyzed by flow cytometry. Results: CD4+Tregs infiltrating ovarian cancer tissues exhibited significantly higher lipid content and lipid uptake capacity compared to conventional CD4+T cells (Tconv) (P < 0.01). Among the ovarian cancer TSNs tested in vitro, CAOV3-derived TSNs most significantly enhanced intracellular lipid content and uptake capacity in CD4+Tregs relative to basal medium (P < 0.05). Furthermore, CAOV3-conditioned medium upregulated PD-1 and CTLA-4 expression in CD4+Tregs (P < 0.05). This was accompanied by a concentration-dependent increase in both lipid accumulation and fluorescent fatty acid analog uptake (P < 0.05). Notably, the fatty acid uptake inhibitor SSO effectively reversed the CAOV3 supernatant-induced lipid accumulation (P < 0.05) in CD4?Tregs and the elevated expression of PD-1 (P < 0.01) and CTLA-4 (P < 0.05), but not by the oxidation inhibitor Etomoxir or the synthesis inhibitor C75. Conclusion: The ovarian cancer microenvironment promotes lipid uptake in CD4+Tregs, leading to intracellular lipid droplet accumulation, which in turn enhances their immunosuppressive function, as evidenced by upregulated PD-1 and CTLA-4 expression. Targeting the fatty acid uptake pathway may represent a potential strategy to reverse Treg-mediated immunosuppression in ovarian cancer. Key words: ovarian cancer; CD4+Tregs; Lipid; PD-1/CTLA-4

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收稿日期:2025-10-16
最后修改日期:2025-11-29
录用日期:2026-01-19
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