N-ethyl-N-nitrosourea (ENU)-induced C-terminal truncation of Runx3 results in autoimmune colitis associated with Th17/Treg imbalance

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Yi-Ting Chen , Yi-Mei Chang , Yu-Ling Chen , Yu-Hsuan Su , Chia-Chi Liao , Tien-Huang Chiang , Wen-Yu Chen , Yu-Chia Su
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Abstract

Inflammatory bowel disease (IBD) is a chronic and progressive inflammatory intestinal disease that affects people around the world. The primary cause of IBD is an imbalance in the host immune response to intestinal flora. Several human genes, including IL10, STAT3, IRGM, ATG16L1, NOD2 and RUNX3, are associated with inappropriate immune responses in IBD. It has been reported that homozygous Runx3-knockout (ko) mice spontaneously develop colitis. However, the high mortality rate in these mice within the first two weeks makes it challenging to study the role of Runx3 in colitis. To address this issue, a spontaneous colitis (SC) mouse model carrying a C-terminal truncated form of Runx3 with Tyr319stop point mutation has been generated. After weaning, SC mice developed spontaneous diarrhea and exhibited prominent enlargement of the colon, accompanied by severe inflammatory cell infiltration. Results of immunofluorescence staining showed massive CD4+ T cell infiltration in the inflammatory colon of SC mice. Colonic IL-17A mRNA expression and serum IL-17A level were increased in SC mice. CD4+ T cells from SC mice produced stronger IL-17A than those from wildtype mice in Th17-skewing conditions in vitro. In addition, the percentages of Foxp3+ Treg cells as well as the RORγt+Foxp3+ Treg subset, known for its role in suppressing Th17 response in the gut, were notably lower in colon lamina propria of SC mice than those in WT mice. Furthermore, transfer of total CD4+ T cells from SC mice, but not from wildtype mice, into Rag1-ko host mice resulted in severe autoimmune colitis. In conclusion, the C-terminal truncated Runx3 caused autoimmune colitis associated with Th17/Treg imbalance. The SC mouse model is a feasible approach to investigate the effect of immune response on spontaneous colitis.

N-乙基-N-亚硝基脲(ENU)诱导的Runx3 C端截短会导致与Th17/Treg失衡相关的自身免疫性结肠炎。
炎症性肠病(IBD)是一种慢性进行性肠道炎症性疾病,影响着世界各地的人们。IBD 的主要病因是宿主对肠道菌群的免疫反应失衡。一些人类基因,包括 IL10、STAT3、IRGM、ATG16L1、NOD2 和 RUNX3,与 IBD 中不适当的免疫反应有关。有报道称,同基因的 Runx3 基因敲除(ko)小鼠会自发患上结肠炎。然而,这些小鼠在头两周内的死亡率很高,因此研究 Runx3 在结肠炎中的作用具有挑战性。为了解决这个问题,研究人员建立了一种自发性结肠炎(SC)小鼠模型,该模型携带有C端截短形式的Runx3,并带有Tyr319stop点突变。断奶后,SC 小鼠出现自发性腹泻,结肠明显肿大,并伴有严重的炎症细胞浸润。免疫荧光染色结果显示,SC 小鼠炎症结肠中存在大量 CD4+ T 细胞浸润。SC 小鼠结肠 IL-17A mRNA 表达和血清 IL-17A 水平均升高。在体外 Th17 筛选条件下,SC 小鼠的 CD4+ T 细胞比野生型小鼠的 CD4+ T 细胞产生更强的 IL-17A。此外,SC 小鼠结肠固有膜中 Foxp3+ Treg 细胞以及 RORγt+Foxp3+ Treg 亚群(因其在抑制肠道 Th17 反应中的作用而闻名)的百分比明显低于 WT 小鼠。此外,将 SC 小鼠而非野生型小鼠的总 CD4+ T 细胞转移到 Rag1-ko 宿主小鼠体内会导致严重的自身免疫性结肠炎。总之,C端截短的Runx3会引起与Th17/Treg失衡相关的自身免疫性结肠炎。SC小鼠模型是研究免疫反应对自发性结肠炎影响的一种可行方法。
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
CiteScore
7.20
自引率
4.30%
发文量
567
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