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Treg-cell depletion promotes chemokine production and accumulation of CXCR3(+) conventional T cells in intestinal tumors

机译:Treg-cell消耗促进趋化因子的生产和积累CXCR3的传统(+)T细胞在肠道肿瘤

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摘要

Colorectal cancer (CRC) is one of the most prevalent tumor types worldwide and tumor-infiltrating T cells are crucial for anti-tumor immunity. We previously demonstrated that Treg cells from CRC patients inhibit transendothelial migration of conventional T cells. However, it remains unclear if local Treg cells affect lymphocyte migration into colonic tumors. By breeding APC(Min/+) mice with depletion of regulatory T cells mice, expressing the diphtheria toxin receptor under the control of the FoxP3 promoter, we were able to selectively deplete Treg cells in tumor-bearing mice, and investigate the impact of these cells on the infiltration of conventional T cells into intestinal tumors. Short-term Treg-cell depletion led to a substantial increase in the frequencies of T cells in the tumors, attributed by both increased infiltration and proliferation of T cells in the Treg-cell-depleted tumors. We also demonstrate a selective increase of the chemokines CXCL9 and CXCL10 in Treg-cell-depleted tumors, which were accompanied by accumulation of CXCR3(+) T cells, and increased IFN- mRNA expression. In conclusion, Treg-cell depletion increases the accumulation of conventional T cells in intestinal tumors, and targeting Treg cells could be a possible anti-tumor immunotherapy, which not only affects T-cell effector functions, but also their recruitment to tumors.
机译:结直肠癌(CRC)是最之一全球流行的肿瘤类型肿瘤浸润T细胞是至关重要的抗肿瘤免疫力。从CRC患者Treg细胞抑制transendothelial传统T的迁移细胞。细胞影响淋巴细胞迁移到结肠肿瘤。损耗的调节性T细胞的小鼠中,表达白喉毒素受体控制FoxP3的启动子,我们可以选择性耗尽Treg细胞肿瘤老鼠,并研究这些细胞的影响在传统的T细胞的渗透肠道肿瘤。导致大幅增加的频率T细胞的肿瘤,由于两种都用增加T的渗透和扩散Treg-cell-depleted细胞肿瘤。演示的选择性增加趋化因子CXCL9在Treg-cell-depleted CXCL10肿瘤,伴随着积累CXCR3 (+) T细胞,以及增加IFN -信使rna表达式。增加传统T的积累细胞在肠道肿瘤,针对Treg可能是一个可能的抗肿瘤细胞免疫疗法,不仅影响t细胞效应功能,而且他们的招聘肿瘤。

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