CCL2-CCR4 轴促进调节性 T 细胞向犬胶质瘤组织的迁移。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-09-01 Epub Date: 2024-07-24 DOI:10.1007/s11060-024-04766-4
W K Panek, R G Toedebusch, B E Mclaughlin, P J Dickinson, J E Van Dyke, K D Woolard, M E Berens, M S Lesniak, B K Sturges, K M Vernau, C Li, J Miska, Christine M Toedebusch
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引用次数: 0

摘要

目的:宠物狗自发性胶质瘤越来越被认为是人类胶质母细胞瘤的一种有价值的转化模型。犬高级别胶质瘤和人类胶质母细胞瘤在分子上有许多相似之处,其中包括抑制抗肿瘤免疫反应的免疫抑制调节性 T 细胞(Tregs)的聚集。在狗体内识别Treg招募的机制可能有助于锁定驱动免疫抑制的细胞群,其结果为在人类患者中开展转化临床研究提供了理论依据。我们的研究小组之前在小鼠正位胶质瘤模型中发现,C-C 矩阵趋化因子 2(CCL2)是一种作用于趋化因子受体 4(CCR4)的胶质瘤衍生 Treg 趋化吸引因子。最近,我们在患有高级别胶质瘤的犬类患者的脑组织中证实了 CCL2 的大量增加:方法:我们使用犬Tregs和患者衍生的犬胶质瘤细胞系(GSC 1110、GSC 0514、J3T-Bg、G06A)进行了一系列体外实验,以研究犬体内的CCL2-CCR4信号轴:我们建立了一种流式细胞术选通策略,用于鉴定和分离犬体内的 FOXP3+ Tregs。犬 CD4 + CD25high T 细胞群高度富集了 FOXP3 和 CCR4 表达,表明它们是真正的 Treg。CCL2或胶质瘤细胞系衍生上清可增强犬Treg的迁移。阻断CCL2-CCR4轴可显著减少犬Tregs的迁移。CCL2 mRNA在所有胶质瘤细胞系中均有表达,当暴露于Tregs而非CD4 +辅助T细胞时,CCL2 mRNA的表达量会增加:我们的研究验证了 CCL2-CCR4 是犬高级别胶质瘤中 Treg-胶质瘤免疫抑制和肿瘤促进的双向轴。
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The CCL2-CCR4 axis promotes Regulatory T cell trafficking to canine glioma tissues.

Purpose: Spontaneously occurring glioma in pet dogs is increasingly recognized as a valuable translational model for human glioblastoma. Canine high-grade glioma and human glioblastomas share many molecular similarities, including the accumulation of immunosuppressive regulatory T cells (Tregs) that inhibit anti-tumor immune responses. Identifying in dog mechanisms responsible for Treg recruitment may afford to target the cellular population driving immunosuppression, the results providing a rationale for translational clinical studies in human patients. Our group has previously identified C-C motif chemokine 2 (CCL2) as a glioma-derived T-reg chemoattractant acting on chemokine receptor 4 (CCR4) in a murine orthotopic glioma model. Recently, we demonstrated a robust increase of CCL2 in the brain tissue of canine patients bearing high-grade glioma.

Methods: We performed a series of in vitro experiments using canine Tregs and patient-derived canine glioma cell lines (GSC 1110, GSC 0514, J3T-Bg, G06A) to interrogate the CCL2-CCR4 signaling axis in the canine.

Results: We established a flow cytometry gating strategy for identifying and isolating FOXP3+ Tregs in dogs. The canine CD4 + CD25high T-cell population was highly enriched in FOXP3 and CCR4 expression, indicating they are bona fide Tregs. Canine Treg migration was enhanced by CCL2 or by glioma cell line-derived supernatant. Blockade of the CCL2-CCR4 axis significantly reduced migration of canine Tregs. CCL2 mRNA was expressed in all glioma cell lines, and expression increased when exposed to Tregs but not CD4 + helper T-cells.

Conclusion: Our study validates CCL2-CCR4 as a bi-directional Treg-glioma immunosuppressive and tumor-promoting axis in canine high-grade glioma.

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