The microRNA expression in crypt-top and crypt-bottom colonic epithelial cell populations demonstrates cell-type specificity and correlates with endoscopic activity in ulcerative colitis.

Ruta Inciuraite, Rima Ramonaite, Juozas Kupcinskas, Indre Dalgediene, Ugne Kulokiene, Vytautas Kiudelis, Greta Varkalaite, Aurelija Zvirbliene, Laimas Virginijus Jonaitis, Gediminas Kiudelis, Andre Franke, Stefan Schreiber, Simonas Juzenas, Jurgita Skieceviciene
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Abstract

Background and aims: Colonic epithelial barrier dysfunction is one of the early events in ulcerative colitis (UC) and microRNAs (miRNAs) participate in its regulation. However, cell type-specific miRNome during UC is still unknown. Thus, we aimed to explore miRNA expression patterns in colon tissue and epithelial cells at active and quiescent UC.

Methods: Small RNA-sequencing in colon tissue, crypt-bottom (CD44+), and crypt-top (CD66a+) colonic epithelial cells from two cohorts of UC patients (n=74) and healthy individuals (n=50) was performed. Data analysis encompassed differential expression, weighted gene co-expression network, correlation, gene-set enrichment analyses.

Results: Differentially expressed colonic tissue miRNAs showed potential involvement in regulation of interleukin-4 and interleukin-13 signalling during UC. As this pathway plays role in intestinal barrier regulation, consecutive analysis of spatially distinct colonic epithelial cell populations was performed. Cell-type (crypt-top and crypt-bottom) specific miRNA expression patterns were identified in both active and quiescent UC. Target genes of differentially expressed epithelial miRNAs at different disease activity were overrepresented in epithelial cell migration and therefore intestinal barrier integrity regulation. The pro-inflammatory miRNA co-expression module M1 correlated with endoscopic disease activity and successfully distinguished active and quiescent UC not only in both epithelial cell populations, but also in the colon tissue. The anti-inflammatory module M2 was specific to crypt-bottom cells and significantly enriched in the quiescent UC patients.

Conclusions: miRNA expression was specific to colonic epithelial cell populations and UC state, reflecting endoscopic disease activity. Irrespective of the UC state, deregulated epithelial miRNAs were associated with regulation of intestinal barrier integrity.

隐窝顶和隐窝底结肠上皮细胞群中的 microRNA 表达显示了细胞类型特异性,并与溃疡性结肠炎的内镜活动相关。
背景和目的:结肠上皮屏障功能障碍是溃疡性结肠炎(UC)的早期症状之一,而微小RNA(miRNA)参与其调控。然而,UC 期间细胞类型特异性的 miRNome 仍然未知。因此,我们旨在探索活动期和静止期 UC 结肠组织和上皮细胞的 miRNA 表达模式:方法:我们对两组 UC 患者(n=74)和健康人(n=50)的结肠组织、隐窝底部(CD44+)和隐窝顶部(CD66a+)结肠上皮细胞进行了小 RNA 测序。数据分析包括差异表达、加权基因共表达网络、相关性、基因集富集分析:结果:差异表达的结肠组织 miRNAs 显示,它们可能参与了 UC 期间白细胞介素-4 和白细胞介素-13 信号的调控。由于该通路在肠屏障调节中发挥作用,因此对空间上不同的结肠上皮细胞群进行了连续分析。研究发现了活动期和静止期 UC 中细胞类型(隐窝顶和隐窝底)特异的 miRNA 表达模式。在不同的疾病活动中,上皮细胞 miRNA 不同表达的靶基因在上皮细胞迁移和肠道屏障完整性调控中的比例过高。促炎 miRNA 共表达模块 M1 与内镜下的疾病活动相关,不仅在两种上皮细胞群中,而且在结肠组织中都能成功区分活动期和静止期 UC。结论:miRNA 的表达对结肠上皮细胞群和 UC 状态具有特异性,反映了内镜下疾病的活动性。无论 UC 状态如何,上皮 miRNA 的失调都与肠屏障完整性的调节有关。
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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