Good Hayley J, Larsen Frederikke, Shin Alice E, Zhang Liyue, Derouet Mathieu, Meriwether David, Worthley Daniel, Reddy Srinivasa T, Wang Timothy C, Asfaha Samuel
Department of Medicine, University of Western Ontario, London, Ontario, Canada; Verspeeten Family Cancer Centre, London Health Sciences Centre, London, Ontario, Canada.
Department of Medicine, Division of Cardiology, UCLA David Geffen School of Medicine, Los Angeles, California.
Cell Mol Gastroenterol Hepatol. 2025;19(6):101469. doi: 10.1016/j.jcmgh.2025.101469. Epub 2025 Jan 28.
BACKGROUND & AIMS: Loss of the tumor suppressor gene Apc in Lgr5+ intestinal stem cells results in aberrant Wnt signaling and colonic tumorigenesis. In the setting of injury, however, we and others have also shown that non-stem cells can give rise to colonic tumors. The mechanism by which inflammation leads to cellular plasticity and cancer, however, remains largely unknown.
RNA expression analysis of Wnt, COX, and Akt signaling was assessed in patients with quiescent or active ulcerative colitis (UC) and patients with UC-associated neoplasia using available datasets. The role of COX signaling in colonic tumorigenesis was examined using epithelial and doublecortin-like kinase 1 (Dclk1)+ cell-specific conditional COX-1 knockout mice and pharmacologic treatment with different nonsteroidal anti-inflammatory drugs.
In this study, we show that prostaglandins and phospho-Akt are key inflammatory mediators that promote stemness in Apc mutant Dclk1+ cells that give rise to colorectal cancer. Moreover, prostaglandin E (PGE) and Akt are increased in colitis in both mice and humans, leading to inflammation-associated dysplasia upon activation of Wnt signaling. Importantly, inhibition of epithelial-derived COX-1 by aspirin or conditional knockout in Dclk1+ cells reduced PGE levels and prevented the development of inflammation-associated colorectal cancer.
Our data shows that epithelial and Dclk1+ cell-derived COX-1 plays an important role in inflammation-associated tumorigenesis. Importantly, low-dose aspirin was effective in chemo-prevention through inhibition of COX-1 that reduced colitis-associated cancer.
Lgr5 + 肠道干细胞中肿瘤抑制基因Apc的缺失会导致Wnt信号异常和结肠肿瘤发生。然而,在损伤情况下,我们和其他人也表明非干细胞可引发结肠肿瘤。然而,炎症导致细胞可塑性和癌症的机制在很大程度上仍不清楚。
使用现有数据集评估静止期或活动期溃疡性结肠炎(UC)患者以及UC相关肿瘤患者中Wnt、COX和Akt信号的RNA表达分析。使用上皮细胞和双皮质素样激酶1(Dclk1)+ 细胞特异性条件性COX - 1基因敲除小鼠以及用不同非甾体抗炎药进行药物治疗,研究COX信号在结肠肿瘤发生中的作用。
在本研究中,我们表明前列腺素和磷酸化Akt是促进产生结直肠癌的Apc突变Dclk1 + 细胞干性的关键炎症介质。此外,前列腺素E(PGE)和Akt在小鼠和人类的结肠炎中均升高,在Wnt信号激活时导致炎症相关的发育异常。重要的是,阿司匹林对上皮来源的COX - 1的抑制或Dclk1 + 细胞中的条件性基因敲除降低了PGE水平,并预防了炎症相关结直肠癌的发生。
我们的数据表明上皮细胞和Dclk1 + 细胞来源的COX - 1在炎症相关肿瘤发生中起重要作用。重要的是,低剂量阿司匹林通过抑制COX - 1有效预防结肠炎相关癌症,从而具有化学预防作用。
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