CD27 signaling inhibits tumor growth and metastasis via CD8 + T cell-independent mechanisms in the B16-F10 melanoma model.

IF 4.6 2区 医学 Q2 IMMUNOLOGY Cancer Immunology, Immunotherapy Pub Date : 2024-08-06 DOI:10.1007/s00262-024-03780-9
Eswara Rao Puppala, Long Wu, Xiaoxuan Fan, Xuefang Cao
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Abstract

CD27 belongs to the tumor necrosis factor receptor superfamily and acts as a co-stimulatory molecule, modulating T and B cell responses. CD27 stimulation enhances T cell survival and effector functions, thus providing opportunities to develop therapeutic strategies. The current study aims to investigate the role of endogenous CD27 signaling in tumor growth and metastasis. CD8 + T cell-specific CD27 knockout (CD8Cre-CD27fl) mice were developed, while global CD27 knockout (KO) mice were also used in our studies. Flow cytometry analyses confirmed that CD27 was deleted specifically from CD8 + T cells without affecting CD4 + T cells, B cells, and HSPCs in the CD8Cre-CD27fl mice, while CD27 was deleted from all cell types in global CD27 KO mice. Tumor growth and metastasis studies were performed by injecting B16-F10 melanoma cells subcutaneously (right flank) or intravenously into the mice. We have found that global CD27 KO mice succumbed to significantly accelerated tumor growth compared to WT controls. In addition, global CD27 KO mice showed a significantly higher burden of metastatic tumor nests in the lungs compared to WT controls. However, there was no significant difference in tumor growth curves, survival, metastatic tumor nest counts between the CD8Cre-CD27fl mice and WT controls. These results suggest that endogenous CD27 signaling inhibits tumor growth and metastasis via CD8 + T cell-independent mechanisms in this commonly used melanoma model, presumably through stimulating antitumor activities of other types of immune cells.

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在 B16-F10 黑色素瘤模型中,CD27 信号通过与 CD8 + T 细胞无关的机制抑制肿瘤生长和转移。
CD27 属于肿瘤坏死因子受体超家族,是一种协同刺激分子,可调节 T 细胞和 B 细胞的反应。CD27 刺激可增强 T 细胞的存活和效应功能,从而为开发治疗策略提供机会。本研究旨在探讨内源性 CD27 信号在肿瘤生长和转移中的作用。我们培育了CD8 + T细胞特异性CD27基因敲除(CD8Cre-CD27fl)小鼠,同时还使用了全基因CD27基因敲除(KO)小鼠。流式细胞术分析证实,在CD8Cre-CD27fl小鼠中,CD27特异性地从CD8 + T细胞中删除,而不影响CD4 + T细胞、B细胞和HSPCs,而在全基因CD27 KO小鼠中,CD27从所有细胞类型中删除。通过向小鼠皮下(右翼)或静脉注射 B16-F10 黑色素瘤细胞,进行了肿瘤生长和转移研究。我们发现,与 WT 对照组相比,CD27 KO 小鼠的肿瘤生长速度明显加快。此外,与 WT 对照组相比,CD27 KO 小鼠肺部转移性肿瘤巢的负担明显增加。然而,CD8Cre-CD27fl小鼠与WT对照组在肿瘤生长曲线、存活率、转移瘤巢数量等方面没有明显差异。这些结果表明,在这种常用的黑色素瘤模型中,内源性 CD27 信号通过 CD8 + T 细胞依赖性机制抑制肿瘤生长和转移,可能是通过刺激其他类型免疫细胞的抗肿瘤活性。
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来源期刊
CiteScore
10.50
自引率
1.70%
发文量
207
审稿时长
1 months
期刊介绍: Cancer Immunology, Immunotherapy has the basic aim of keeping readers informed of the latest research results in the fields of oncology and immunology. As knowledge expands, the scope of the journal has broadened to include more of the progress being made in the areas of biology concerned with biological response modifiers. This helps keep readers up to date on the latest advances in our understanding of tumor-host interactions. The journal publishes short editorials including "position papers," general reviews, original articles, and short communications, providing a forum for the most current experimental and clinical advances in tumor immunology.
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