首页> 外文期刊>Inflammatory bowel diseases >Genome-wide gene expression analysis of mucosal colonic biopsies and isolated colonocytes suggests a continuous inflammatory state in the lamina propria of patients with quiescent ulcerative colitis.
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Genome-wide gene expression analysis of mucosal colonic biopsies and isolated colonocytes suggests a continuous inflammatory state in the lamina propria of patients with quiescent ulcerative colitis.

机译:粘膜结肠活检和分离的结肠细胞的全基因组基因表达分析表明,静止期溃疡性结肠炎患者固有层的持续炎性状态。

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BACKGROUND: Genome-wide gene expression (GWGE) profiles of mucosal colonic biopsies have suggested the existence of a continuous inflammatory state in quiescent ulcerative colitis (UC). The aim of this study was to use DNA microarray-based GWGE profiling of mucosal colonic biopsies and isolated colonocytes from UC patients and controls in order to identify the cell types responsible for the continuous inflammatory state. METHODS: Adjacent mucosal colonic biopsies were obtained endoscopically from the descending colon in patients with active UC (n = 8), quiescent UC (n = 9), and with irritable bowel syndrome (controls, n = 10). After isolation of colonocytes and subsequent extraction of total RNA, GWGE data were acquired using Human Genome U133 Plus 2.0 GeneChip Array (Affymetrix, Santa Clara, CA). Data analysis was carried out by principal component analysis and projection to latent structure-discriminant analysis using the SIMCA-P 11 software (Umetrics, Umea, Sweden). RESULTS: A clear separation between active UC, quiescent UC, and control biopsies were found, whereas the model for the colonocytes was unable to distinguish between quiescent UC and controls. The differentiation between quiescent UC and control biopsies was governed by unique profiles containing gene expressions with significant fold changes. These primarily belonged to the family of homeostatic chemokines, revealing a plausible explanation for the abnormal regulated innate immune response seen in patients with UC. CONCLUSIONS: This study has demonstrated the presence of a continuous inflammatory state in quiescent UC, which seems to reflect an altered gene expression profile of lamina propria cells.
机译:背景:粘膜结肠活检的全基因组基因表达(GWGE)资料表明,静态溃疡性结肠炎(UC)中存在持续的炎症状态。这项研究的目的是使用基于DNA芯片的GWGE粘膜结肠活检以及来自UC患者和对照的分离的结肠细胞,以鉴定造成持续炎症状态的细胞类型。方法:对活动性UC(n = 8),静止性UC(n = 9)和肠易激综合征(对照组,n = 10)的患者,通过内镜从降结肠结肠镜检取粘膜结肠活检。分离结肠细胞并随后提取总RNA后,使用人类基因组U133 Plus 2.0基因芯片阵列(Affymetrix,圣克拉拉,加利福尼亚州)获取GWGE数据。使用SIMCA-P 11软件(Umetrics,Umea,瑞典),通过主成分分析和投影到潜在结构判别分析进行数据分析。结果:发现活动性UC,静态UC和对照活组织检查物之间存在清晰的分离,而结肠细胞模型无法区分静态UC和对照。静态UC和对照活检之间的区别由包含具有显着倍数变化的基因表达的独特特征决定。这些主要属于体内趋化因子家族,为在UC患者中观察到的异常调节的先天免疫应答提供了合理的解释。结论:这项研究证明了静态UC中存在持续的炎症状态,这似乎反映了固有层细胞基因表达谱的改变。

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