葡聚糖硫酸钠猪结肠炎模型中神经活性受体的转录组学评估

M. Ryan, J.V. O'Doherty, Torres Sweeney
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摘要

肠道神经系统(ENS)与局部免疫系统双向互动,对胃肠道(GI)内的炎症做出反应。在之前对相同样本的研究中,发现了几个基因靶点在受到葡聚糖硫酸钠(DSS)挑战的猪发炎结肠组织中的不同表达。此外,基础 DSS 组动物的生长速度降低,粪便和病理评分增加,有益类群的相对丰度降低,有害细菌增加。虽然先天性免疫反应和屏障功能的变化在炎症性肠病(IBD)中被广泛提及,但炎症对肠道神经系统(ENS)局部结构的影响却鲜为人知。因此,本研究的目的是(1) 评估来自相同猪只结肠组织的 RNA 中一系列功能多样的神经活性受体、转运体和神经营养因子的表达;(2) 研究这些神经活性成分与炎症、屏障功能和基质重塑靶点之间的关联。成年猪被分成两个实验组:(1) 基础饮食组(n = 10);(2) 基础饮食 + DSS 组(n = 11)。猪每天口服一次 DSS,连续四天,然后人道处死。收集结肠组织进行基因表达分析。本研究中评估的大多数靶点的基因表达水平都很低,甚至在某些情况下无法通过 QPCR 检测到,其中包括多巴胺受体 DRD5 和血清素受体 HTR3A。与基础组相比,多巴胺受体(DRD1、DRD3、DRD4)、血清素受体(HTR4)和其他选定的神经活性受体(GRM7、GABRA2)在 DSS 挑战动物体内下调(p < 0.05)。最值得注意的是,DRD2 上调了四倍,这表明该受体参与了一个活跃的过程(p < 0.05)。与(以前发表的)来自相同样本的基因表达数据的关系表明,DRD1 和 DRD2 受不同途径的影响,也可能与基质重塑相互关联,更具体地说,与上皮细胞向间充质转化相关的基因(CDH1、CDH2、IL6、IL13、IL10、MMP1、MMP2)也有关联,而上皮细胞向间充质转化是 IBD 发病机制中一个重要的纤维化过程。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Transcriptomic Evaluation of Neuroactive Receptors in the Colon of a Dextran Sodium Sulphate Pig Model of Colitis
The enteric nervous system (ENS) interacts bidirectionally with the local immune system, responding to inflammation within the gastrointestinal (GI) tract. In a previous study the same samples, several gene targets were identified as being differentially expressed in the inflamed colonic tissue of pigs challenged with dextran sodium sulphate (DSS). Additionally, animals in the basal DSS group, exhibited reduced growth and increased fecal and pathology scores, while the relative abundance of beneficial taxa was reduced and harmful bacteria increased. While changes in the innate immune response and barrier function are widely cited regarding inflammatory bowel disease (IBD), the effects of inflammation on the local structures of the enteric nervous system (ENS) are less well understood. Hence, the objectives of this study were to: (1) evaluate the expression of a range of functionally diverse neuroactive receptors, transporters and neurotrophic factors in RNA derived from the colonic tissue from the same pigs; (2) examine associations with these neuroactive components and inflammatory, barrier function and matrix remodeling targets. Mature pigs were split into two experimental groups: (1) basal diet (n = 10); (2) basal diet + DSS (n = 11). The pigs were orally challenged with DSS once daily for four days and sacrificed humanely. Colonic tissue was collected for gene expression analysis. Most of the targets evaluated in this study were present at low levels or in some cases were undetectable by QPCR, including the dopamine receptor DRD5 and the serotonin receptor HTR3A. The dopamine receptors (DRD1, DRD3, DRD4), serotonin receptor (HTR4), and other selected neuroactive receptors (GRM7, GABRA2) were down-regulated in the DSS-challenged animals relative to the basal group (p < 0.05). Most notably, DRD2, was up-regulated four-fold, suggesting an active process involving this receptor (p < 0.05). Relationships with (previously published) gene expression data from the same samples suggest that DRD1 and DRD2 are influenced by different pathways and may also be interlinked with matrix remodeling and, more specifically, genes relevant to the epithelial to mesenchymal transition (CDH1, CDH2, IL6, IL13, IL10, MMP1, MMP2) an important fibrotic process in the pathogenesis of IBD.
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