PARP1 inactivation increases regulatory T / Th17 cell proportion in intestinal inflammation. Role of HMGB1

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Roberta Vitali , Flavia Novelli , Francesca Palone , Salvatore Cucchiara , Laura Stronati , Claudio Pioli
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Abstract

Inflammatory bowel diseases (IBD) are chronic relapsing disorders with increasing prevalence. Knowledge gaps still limit the possibility to develop more specific and effective therapies. Using a dextran sodium sulfate colitis mouse model, we found that inflammation increased the total number and altered the frequencies of leukocytes within colon mesenteric lymph nodes (cMLNs). Although the inflammation reduced the frequency of regulatory T (Treg) cells, their absolute numbers were increased. Increased frequency of colitogenic Th17 cells was also observed. Noteworthy, untreated mice lacking Poly(ADP-ribose)-Polimerase-1 functional gene (PARP-1KO) displayed higher frequency of Treg cells and lower percentage of Th17 cells in cMLNs. In colitic PARP-1KO mice the inflammation driven expansion of the Foxp3 Treg population was more pronounced than in WT mice. Conversely, colitis increased Th17 cells to a lower extent in PARP-1KO mice compared with WT mice, resulting in a more protective Treg/Th17 cell ratio. Consequently PARP-1KO mice developed less severe colitis with reduced expression of inflammatory cytokines. In ex vivo experiments PARP-1KO and WT CD11c dendritic cells (DCs) promoted naïve CD4 T cell differentiation differently, the former sustaining more efficiently the generation of Treg cells, the latter that of Th17 cells. Addition of HMGB1 B box or of dipotassium glycyrrhizate, which sequesters extracellular HMGB1, revealed a role for this alarmin in the regulation exerted by PARP-1 on the stimulating vs. tolerogenic function of DCs during colitis. Moreover, a higher percentage of CD11c DC from PARP-1KO mice expressed CD103, a marker associated with the ability of DC to induce Treg cells, compared with WT DC. Conversely, PARP-1KO DC were including a reduced percentage of CX3CR1+ DC, described to induce Th17 cells. These findings were observed in both splenic and colon lamina propria DC.

PARP1 失活会增加肠道炎症中调节性 T 细胞/Th17 细胞的比例。HMGB1 的作用
炎症性肠病(IBD)是一种慢性复发性疾病,发病率越来越高。知识上的差距仍然限制着开发更具体、更有效疗法的可能性。通过使用葡聚糖硫酸钠结肠炎小鼠模型,我们发现炎症增加了结肠肠系膜淋巴结(cMLNs)内白细胞的总数并改变了其频率。虽然炎症降低了调节性 T(Treg)细胞的频率,但其绝对数量却增加了。此外,还观察到结肠Th17细胞的频率增加。值得注意的是,缺乏聚(ADP-核糖)聚合酶-1 功能基因(PARP-1KO)的未处理小鼠在 cMLNs 中显示出较高的 Treg 细胞频率和较低的 Th17 细胞百分比。在患有结肠炎的 PARP-1KO 小鼠中,炎症导致的 Foxp3 Treg 群体的扩大比 WT 小鼠更明显。相反,与 WT 小鼠相比,PARP-1KO 小鼠结肠炎增加 Th17 细胞的程度较低,从而使 Treg/Th17 细胞的比例更具保护性。因此,PARP-1KO 小鼠患结肠炎的程度较轻,炎性细胞因子的表达也较少。在体外实验中,PARP-1KO 和 WT CD11c 树突状细胞(DCs)对幼稚 CD4 T 细胞分化的促进作用不同,前者能更有效地维持 Treg 细胞的生成,后者则能维持 Th17 细胞的生成。加入 HMGB1 B 盒或甘草酸二钾(能封闭细胞外的 HMGB1)后,发现这种警戒素在 PARP-1 对结肠炎期间 DCs 的刺激与耐受功能的调节中发挥作用。此外,与 WT DC 相比,PARP-1KO 小鼠的 CD11c DC 表达 CD103 的比例更高,而 CD103 是 DC 诱导 Treg 细胞能力的相关标记。相反,PARP-1KO小鼠的DC中CX3CR1+ DC比例较低,而CX3CR1+ DC被认为能诱导Th17细胞。这些发现在脾脏和结肠固有层DC中都能观察到。
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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