An Upstream RUNX3 Enhancer, eR3 (−18m/−28h), Regulates the Development of Gut-Associated Anti-Tumorigenic CD8+CD103+ Cytotoxic T Lymphocytes in Mouse and Human

IF 1.3 4区生物学 Q4 CELL BIOLOGY

Genes to Cells Pub Date : 2025-10-19 DOI:10.1111/gtc.70052

Giselle Sek Suan Nah, Junichi Matsuo, Avinash Govind Bahirvani, Shunichi Kimura, Desmond Wai Loon Chin, King Pan Ng, Cai Ping Koh, Michelle Meng Huang Mok, Chelsia Qiuxia Wang, Vinay Tergaonker, Dominic C. Voon, Kazuyoshi Kohu, Sawako Muroi, Jizhong Shi, Shuizhou Yu, Md. Zakir Hossain, Wei-Siang Liau, Cao Thi Ngoc Phuong, Takaomi Sanda, Judith Marsman, Julia Horsfield, Hilde Cheroutre, Yiong Huak Chan, Brendan Pang, Pei Yi Chong, Richie Soong, Daniel G. Tenen, Yoichi Maekawa, Byrappa Venkatesh, Yoshiaki Ito, Ichiro Taniuchi, Motomi Osato

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Abstract

The RUNX3 gene is frequently involved in a variety of cancers and immunological diseases. Despite such widespread association with human diseases, the transcriptional regulation of RUNX3 remains elusive. Here we report the identification of an enhancer for Runx3, eR3(−18m/−28h), by employing a combination of in silico prediction and in vivo verification using zebrafish and mouse models. eR3 is active in CD8⁺CD103 (integrin α_E)⁺ cytotoxic T lymphocytes (CTLs) that reside in the intestinal epithelium via their interaction with the CD103 ligand, E-cadherin, on epithelial cells. Removal of eR3(−18m) specifically in CD8 T cells compromised the suppression of tumorigenesis in murine cancer models. In humans, single nucleotide polymorphisms (SNPs) in eR3(−28h) were overrepresented and were associated with weakened CTL activity in colorectal cancer patients. Together, our results indicate that eR3 plays a role in immune surveillance against gut-associated tumors by upregulating RUNX3 expression in specific CTLs.

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上游RUNX3增强子eR3（−18m/−28h）调节小鼠和人肠道相关抗肿瘤CD8+CD103+细胞毒性T淋巴细胞的发育

RUNX3基因经常与多种癌症和免疫疾病有关。尽管与人类疾病有如此广泛的关联，RUNX3的转录调控仍然难以捉摸。在这里，我们报告了Runx3， eR3的增强子（−18m/−28h）的鉴定，采用计算机预测和斑马鱼和小鼠模型的体内验证相结合。eR3通过与上皮细胞上的CD103配体e -钙粘蛋白相互作用，在肠上皮内的CD8+CD103（整合素αE）+细胞毒性T淋巴细胞（ctl）中具有活性。在小鼠癌症模型中，特异性去除CD8 T细胞中的eR3（−18m）破坏了对肿瘤发生的抑制。在人类中，eR3（−28小时）的单核苷酸多态性（snp）被过度代表，并且与结直肠癌患者的CTL活性减弱有关。总之，我们的研究结果表明，eR3通过上调RUNX3在特定ctl中的表达，在针对肠道相关肿瘤的免疫监视中发挥作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Genes to Cells 生物-细胞生物学

CiteScore

3.40

自引率

0.00%

发文量

审稿时长

3 months

期刊介绍： Genes to Cells provides an international forum for the publication of papers describing important aspects of molecular and cellular biology. The journal aims to present papers that provide conceptual advance in the relevant field. Particular emphasis will be placed on work aimed at understanding the basic mechanisms underlying biological events.