肿瘤细胞释放的自噬体(TRAPs)诱导 PD-L1 修饰的 NETs,抑制 T 细胞功能,促进乳腺癌肺转移。
Tumor cell-released autophagosomes (TRAPs) induce PD-L1-decorated NETs that suppress T-cell function to promote breast cancer pulmonary metastasis.
机构信息
Jiangsu Provincial Key Laboratory of Critical Care Medicine, Department of Microbiology and Immunology, School of Medicine, Southeast University, Nanjing, Jiangsu, China.
Department of Laboratory Medicine, Yantai Yuhuangding Hospital, Yantai, Shandong, China.
出版信息
J Immunother Cancer. 2024 Jun 26;12(6):e009082. doi: 10.1136/jitc-2024-009082.
BACKGROUND
Lung metastasis is the primary cause of breast cancer-related mortality. Neutrophil extracellular traps (NETs) are involved in the progression of breast cancer. However, the mechanism of NET formation is not fully understood. This study posits that tumor cell-released autophagosomes (TRAPs) play a crucial role in this process.
METHODS
TRAPs were isolated from breast cancer cell lines to analyze their impact on NET formation in both human and mouse neutrophils. The study used both in vitro and in vivo models, including Toll-like receptor 4 (TLR4/) mice and engineered breast cancer cell lines. Immunofluorescence, ELISA, Western blotting, RNA sequencing, and flow cytometry were employed to dissect the signaling pathways leading to NET production and to explore their immunosuppressive effects, particularly focusing on the impact of NETs on T-cell function. The therapeutic potential of targeting TRAP-induced NETs and their immunosuppressive functions was evaluated using DNase I and αPD-L1 antibodies. Clinical relevance was assessed by correlating circulating levels of TRAPs and NETs with lung metastasis in patients with breast cancer.
RESULTS
This study showed that TRAPs induced the formation of NETs in both human and mouse neutrophils by using the high mobility group box 1 and activating the TLR4-Myd88-ERK/p38 signaling axis. More importantly, PD-L1 carried by TRAP-induced NETs inhibited T-cell function in vitro and in vivo, thereby contributing to the formation of lung premetastatic niche (PMN) immunosuppression. In contrast, KD-4T1 breast tumors with decreased circulating TRAPs in vivo reduced the formation of NETs, which in turn attenuated the immunosuppressive effects in PMN and resulted in a reduction of breast cancer pulmonary metastasis in murine models. Moreover, treatment with αPD-L1 in combination with DNase I that degraded NETs restored T-cell function and significantly reduced tumor metastasis. TRAP levels in the peripheral blood positively correlated with NET levels and lung metastasis in patients with breast cancer.
CONCLUSIONS
Our results demonstrate a novel role of TRAPs in the formation of PD-L1-decorated NETs, which may provide a new strategy for early detection and treatment of pulmonary metastasis in patients with breast cancer.
背景
肺转移是乳腺癌相关死亡的主要原因。中性粒细胞胞外诱捕网(NETs)参与了乳腺癌的进展。然而,NET 形成的机制尚不完全清楚。本研究假设肿瘤细胞释放的自噬体(TRAPs)在这个过程中起着关键作用。
方法
从乳腺癌细胞系中分离 TRAPs,分析其对人源和鼠源中性粒细胞中 NET 形成的影响。该研究使用了体内外模型,包括 Toll 样受体 4(TLR4)/小鼠和工程化的乳腺癌细胞系。免疫荧光、ELISA、Western blot、RNA 测序和流式细胞术用于剖析导致 NET 产生的信号通路,并探索其免疫抑制作用,特别是聚焦 NET 对 T 细胞功能的影响。使用 DNAse I 和 αPD-L1 抗体评估靶向 TRAP 诱导的 NETs 及其免疫抑制功能的治疗潜力。通过将循环 TRAPs 和 NETs 水平与乳腺癌患者的肺转移相关联,评估其临床相关性。
结果
本研究表明,TRAPs 通过高迁移率族框 1(HMGB1)并激活 TLR4-Myd88-ERK/p38 信号通路,在人源和鼠源中性粒细胞中诱导 NET 形成。更重要的是,TRAP 诱导的 NET 上的 PD-L1 抑制了体外和体内的 T 细胞功能,从而促进了肺前转移龛(PMN)免疫抑制的形成。相比之下,体内 KD-4T1 乳腺癌肿瘤中循环 TRAPs 的减少降低了 NET 的形成,进而减弱了 PMN 中的免疫抑制作用,并导致小鼠模型中乳腺癌肺转移的减少。此外,用αPD-L1 联合降解 NET 的 DNAse I 治疗恢复了 T 细胞功能,并显著降低了肿瘤转移。乳腺癌患者外周血中的 TRAP 水平与 NET 水平和肺转移呈正相关。
结论
我们的研究结果表明 TRAPs 在形成 PD-L1 修饰的 NETs 中发挥了新的作用,这可能为乳腺癌患者肺转移的早期检测和治疗提供新的策略。
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