IL-15 的过表达通过 NK1.1+细胞促进自发性乳腺癌模型中的肿瘤破坏。

Overexpression of IL-15 promotes tumor destruction via NK1.1+ cells in a spontaneous breast cancer model.

机构信息

Department of Pathology and Molecular Medicine, McMaster Immunology Research Center (MIRC), McMaster University, Hamilton, Canada.

出版信息

BMC Cancer. 2015 Apr 16;15:293. doi: 10.1186/s12885-015-1264-3.

DOI:10.1186/s12885-015-1264-3

PMID:25879689

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4428091/

Abstract

BACKGROUND

Natural Killer (NK) cells play an important role in tumor prevention, but once tumors form, the numbers as well as the cytotoxic functions of NK cells are reduced. IL-15 is a cytokine that increases and activates NK cells. Here we will examine the anti-tumor role of IL-15 in a spontaneous breast cancer model.

METHODS

To achieve this, Polyoma Middle T (MT) mice that form spontaneous breast cancer were crossed with mice that either overexpress IL-15 (IL-15 transgenic (TG)) or mice that lack IL-15 (IL-15 knockout (KO)). We compared survival curves and tumor formation in IL-15 KO/MT, MT and IL-15 TG/MT groups. In addition, the phenotype, activation and contribution of NK cells and CD8 T cells to tumor formation were examined in each of these mouse strains via flow cytometry, ELISA, adoptive transfer and antibody depletion experiments.

RESULTS

IL-15KO/MT tumors formed and progressed to endpoint more quickly than MT tumors. These tumors displayed little apoptosis and poor CD8 T cell infiltration. In contrast, IL-15 TG/MT mice had increased survival and the tumors displayed extensive cell death, high proportions of activated NK cells and a higher infiltration of CD8 T cells than MT tumors. CD8 T cells in IL-15 TG/MT tumors were capable of secreting IFNγ, possessed markers of memory, did not display an exhausted phenotype and were frequently NK1.1+. Long-term antibody depletion studies in IL-15 TG/MT mice revealed that NK1.1+, but not CD8 T cells, were critical for tumor destruction. Lastly, human NK cells, when exposed to a similar cytokine environment as that found in IL-15TG/MT tumors, were capable of killing human breast cancer cells.

CONCLUSIONS

This study reveals that high levels of IL-15 can promote tumor destruction and reduce metastasis in breast cancer via effects on NK1.1+ cells. Our results suggest that strategies aimed at increasing NK cell activation may be effective against solid epithelial cancers.

摘要

背景

自然杀伤 (NK) 细胞在肿瘤预防中发挥着重要作用，但一旦肿瘤形成，NK 细胞的数量和细胞毒性功能都会降低。白细胞介素 15 (IL-15) 是一种能够增加和激活 NK 细胞的细胞因子。在这里，我们将在自发性乳腺癌模型中研究 IL-15 的抗肿瘤作用。

方法

为此，我们将形成自发性乳腺癌的多瘤病毒中间 T (MT) 小鼠与过表达 IL-15 的小鼠（IL-15 转基因 (TG)）或缺乏 IL-15 的小鼠（IL-15 敲除 (KO)）进行杂交。我们比较了 IL-15 KO/MT、MT 和 IL-15 TG/MT 组的生存曲线和肿瘤形成情况。此外，我们通过流式细胞术、ELISA、过继转移和抗体耗竭实验，检查了每种小鼠品系中 NK 细胞和 CD8 T 细胞的表型、激活和对肿瘤形成的贡献。

结果

IL-15 KO/MT 肿瘤形成并更快地进展到终点，而 MT 肿瘤则形成较慢。这些肿瘤显示出很少的细胞凋亡和较差的 CD8 T 细胞浸润。相比之下，IL-15 TG/MT 小鼠的存活率增加，肿瘤显示出广泛的细胞死亡、高比例的活化 NK 细胞和比 MT 肿瘤更高的 CD8 T 细胞浸润。IL-15 TG/MT 肿瘤中的 CD8 T 细胞能够分泌 IFNγ，具有记忆标记物，不显示衰竭表型，并且经常是 NK1.1+。在 IL-15 TG/MT 小鼠中进行的长期抗体耗竭研究表明，NK1.1+，而不是 CD8 T 细胞，对肿瘤破坏至关重要。最后，当人类 NK 细胞暴露于类似于 IL-15 TG/MT 肿瘤中发现的细胞因子环境时，能够杀死人类乳腺癌细胞。

结论

这项研究揭示了高水平的 IL-15 通过对 NK1.1+细胞的作用，能够促进乳腺癌的肿瘤破坏和减少转移。我们的结果表明，旨在增加 NK 细胞激活的策略可能对实体上皮癌有效。

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IL-15 的过表达通过 NK1.1+细胞促进自发性乳腺癌模型中的肿瘤破坏。

Overexpression of IL-15 promotes tumor destruction via NK1.1+ cells in a spontaneous breast cancer model.

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BACKGROUND

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RESULTS

CONCLUSIONS

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